TOXICOLOGICAL PROFILE FOR HEXACHLOROETHANE Prepared by: Sciences International, Inc. Under Subcontract to: Research Triangle Institute Under Contract No. 205-93-0606 Prepared for: U.S. DEPARTMENT OF HEALTH AND HUMAN SERVICES Public Health Service Agency for Toxic Substances and Disease Registry September 1997 HEXACHLOROETHANE DISCLAIMER The use of company or product name(s) is for identification only and does not imply endorsement by the Agency for Toxic Substances and Disease Registry. CAT. FOR PUBLIC HEALTH HEXACHLOROETHANE iii UPDATE STATEMENT | Toxicological profiles are revised and republished as necessary, but no less than once every three years. For information regarding the update status of previously released profiles, contact ATSDR at: Agency for Toxic Substances and Disease Registry / pb | ° % 2 Division of Toxicology/Toxicology Information Branch fe ° 7 T L 9 1600 Clifton Road NE, E-29 [1 Cr Atlanta, Georgia 30333 7 4 7 PUBL FOREWORD This toxicological profile is prepared in accordance with guidelines* developed by the Agency for Toxic Substances and Disease Registry (ATSDR) and the Environmental Protection Agency (EPA). The original guidelines were published in the Federal Register on April 17, 1987. Each profile will be revised and republished as necessary. The ATSDR toxicological profile succinctly characterizes the toxicologic and adverse health effects information for the hazardous substance described therein. Each peer-reviewed profile identifies and reviews the key literature that describes a hazardous substance's toxicologic properties. Other pertinent literature is also presented, but is described in less detail than the key studies. The profile is not intended to be an exhaustive document; however, more comprehensive sources of specialty information are referenced. The focus of the profiles is on health and toxicologic information; therefore, each toxicological profile begins with a public health statement that describes, in nontechnical language, a substance's relevant toxicological properties. Following the public health statement is information concerning levels of significant human exposure and, where known, significant health effects. The adequacy of information to determine a substance's health effects is described in a health effects summary. Data needs that are of significance to protection of public health are identified by ATSDR and EPA. Each profile includes the following: (A) The examination, summary, and interpretation of available toxicologic information and epidemiologic evaluations on a hazardous substance to ascertain the levels of significant human exposure for the substance and the associated acute, subacute, and chronic health effects; (B) A determination of whether adequate information on the health effects of each substance is available or in the process of development to determine levels of exposure that present a significant risk to human health of acute, subacute, and chronic health effects; and (C) Where appropriate, identification of toxicologic testing needed to identify the types or levels of exposure that may present significant risk of adverse health effects in humans. The principal audiences for the toxicological profiles are health professionals at the Federal, State, and local levels; interested private sector organizations and groups; and members of the public. This profile reflects ATSDR’s assessment of all relevant toxicologic testing and information that has been peer-reviewed. Staff of the Centers for Disease Control and Prevention and other Federal scientists have also reviewed the profile. In addition, this profile has been peer-reviewed by a nongovernmental panel and was made available for public review. Final responsibility for the contents and views expressed in this toxicological profile resides with ATSDR. Go Sh David Satcher, M.D., Ph.D. Administrator Agency for Toxic Substances and Disease Registry vi *Legislative Background The toxicological profiles are developed in response to the Superfund Amendments and Reauthorization Act (SARA) of 1986 (Public Law 99-499) which amended the Comprehensive Environmental Response, Compensation, and Liability Act of 1980 (CERCLA or Superfund). Section 211 of SARA also amended Title 10 of the U. S. Code, creating the Defense Environmental Restoration Program. Section 2704(a) of Title 10 of the U. S. Code directs the Secretary of Defense to notify the Secretary of Health and Human Services of not less than 25 of the most commonly found unregulated hazardous substances at defense facilities. Section 2704(b) of Title 10 of the U. S. Code directs the Administrator of the Agency for Toxic Substances and Disease Registry (ATSDR) to prepare a toxicological profile for each substance on the list provided by the Secretary of Defense under subsection (b). HEXACHLOROETHANE vii CONTRIBUTORS CHEMICAL MANAGER(S)/AUTHOR(S): Cassandra Smith-Simon, M.S. ATSDR, Division of Toxicology, Atlanta, GA Joyce M. Donohue, Ph.D. Life Systems, Inc., Arlington, VA Carol Eisenmann, Ph.D. Sciences International, Inc., Alexandria, VA THE PROFILE HAS UNDERGONE THE FOLLOWING ATSDR INTERNAL REVIEWS: 1. Green Border Review. Green Border review assures the consistency with ATSDR policy. 2 Health Effects Review. The Health Effects Review Committee examines the health effects chapter of each profile for consistency and accuracy in interpreting health effects and classifying end points. 3 Minimal Risk Level Review. The Minimal Risk Level Workgroup considers issues relevant to substance-specific minimal risk levels (MRLs), reviews the health effects database of each profile, and makes recommendations for derivation of MRLs. HEXACHLOROETHANE ix PEER REVIEW A peer review panel was assembled for Hexachloroethane. The panel consisted of the following members: 1. Mr. Bruce Jacobs, General Physics Corporation, Edgewood, MD 2 Mr. Lyman Skory, Private Consultant, Midland, Michigan 3. Dr. Peter Van Voris, Senior Program Manager, Richland, Washington These experts collectively have knowledge of hexachloroethane's physical and chemical properties, toxicokinetics, key health end points, mechanisms of action, human and animal exposure, and quantification of risk to humans. All reviewers were selected in conformity with the conditions for peer review specified in Section 104(I)(13) of the Comprehensive Environmental Response, Compensation, and Liability Act, as amended. Scientists from the Agency for Toxic Substances and Disease Registry (ATSDR) have reviewed the peer reviewers’ comments and determined which comments will be included in the profile. A listing of the peer reviewers’ comments not incorporated in the profile, with a brief explanation of the rationale for their exclusion, exists as part of the administrative record for this compound. A list of databases reviewed and a list of unpublished documents cited are also included in the administrative record. The citation of the peer review panel should not be understood to imply its approval of the profile's final content. The responsibility for the content of this profile lies with the ATSDR. HEXACHLOROETHANE Xi CONTENTS FOREWORD) «ovis simumbes samnmusnns sonar sti s0nasosssasessveannoss hb rssasissssins v CONTRIBUTORS ovo cvimmnr sc iduhins 18a sasssssnnnmnnt shins ss 4RBansss smmnnnoss. vii PEER REVIEW ..uiuss sr iasnmmens sons sss tsassstanonssssoannresi ti@uassessnsvnrsss ix LISTOF FIGURES .....oiviiivtassvnnrtseesssnsasenssnesssosnssnssresssasnsosnnnnns XV LIST OF TABLES ..ccunvsssrtmmmusvrmnnsnit s4ouausns tmasssssanonnnsit inSusssssemon xvii 1. PUBLIC HEALTH STATEMENT ... i suusnsrrovavnusss rds tits ssnnsunpssecnnnmess ens 1 1.1 WHATIS HEXACHLOROETHANE? ...... iia 2 1.2 WHAT HAPPENS TO HEXACHLOROETHANE WHEN IT ENTERS THE ENVIRONMENT © ott tee ee ee eee eee eee eee 2 1.3 HOW MIGHT I BE EXPOSED TO HEXACHLOROETHANE? .................oonnn 4 1.4 HOW CAN HEXACHLOROETHANE ENTER AND LEAVE MY BODY? ............. 5 1.5 HOW CAN HEXACHLOROETHANE AFFECT MY HEALTH? ...................... 5 16 1S THERE A MEDICAL TEST TO DETERMINE WHETHER I HAVE BEEN EXPOSED TO HEXACHLOROETHANE? . otitis eases 6 17 WHAT RECOMMENDATIONS HAS THE FEDERAL GOVERNMENT MADE TO PROTECT HUMAN HEALTH? otitis 7 1.8 WHERE CAN I GET MORE INFORMATION? .... o.oo 8 HEALTH EPFEUTS ois es vaumsissisaasssssansassnssnsnnts sassassissssasensss noe 9 21 INTRODUCTION ities ees 9 79 DISCUSSION OF HEALTH EFFECTS BY ROUTE OF EXPOSURE .................. 9 2.2.1 Inhalation EXPOSUIE ......iiiiinnn reins 11 22.1.1 Death ooo ote 11 22.12 SystemicEffects ..........ccvvviiiiiiiiiiii ees 19 2.2.1.3 Immunological and Lymphoreticular Effects ........................ 24 2.2.1.4 Neurological Effects .............oviiiiiniiiini ian 25 2.2.1.5 Reproductive Effects .............ooiiiiiiii ee 26 2.2.1.6 Developmental Effects .............coiiiiinrinnnin 26 2.2.17 Genotoxic Effects .... overt 26 2.2.1.8 CANCEL «vee ee eee ee eee ee 27 222 Oral EXpoSUrE .......covviitter errata 27 D221 Death... urs rE E EERE ERA Es Sen rs AGAR EE AE REDE SS 27 2222 SystemicEffects .......... vrei 28 2.2.2.3 Immunological and Lymphoreticular Effects ........................ 45 2224 Neurological Effects ............ ccna. 46 2.2.2.5 Reproductive Effects . .........cooiiiiiiiiiiiiii 47 2.2.2.6 Developmental Effects .............ccoiiiiiiiiiiiiiiiiinn 47 2.227 GenotoxiC Effects .... ovine 48 BIDS CAICEL overs nvmanr sss aaa diasseamnnsroansmmnssbituuBsidssennns 48 223 Dermal EXPOsSuIe .......covvssssnmnrvenassccnesssansnsssssssnsverannns 49 223.1 Death «ott 49 HEXACHLOROETHANE Xii 223.2 Systemic Effects ................ 50 2.2.3.3 Immunological and Lymphoreticular Effects ........................ 53 2.2.3.4 Neurological Effects ................... 53 2.2.3.5 Reproductive Effects ..................... 54 2.2.3.6 Developmental Effects ....................... 0. 54 2.2.3.7 Genotoxic Effects ........... 54 2238 CanCer ....... 54 23 TOXICOKINETICS «viii ier creer tse taasas eee 54 23.1 ADBSOIPHON oo 55 23.1.1 Inhalation EXposure ..................... 5s 23.1.2 Oral EXpOSUIe ............ooiunaan i 55 23.1.3 Dermal EXposure ....................c.oiiiiii 56 2.3.2 Distribution... 57 2.3.2.1 Inhalation EXposure ..................... 57 2322 Oral EXpOSUre ...............ouuuuunaneaaai iii, 57 2.3.23 Dermal Exposure ................ 58 2.3.2.4 Other Routes of Exposure ...................... 58 233 Metabolism ....... c.count 59 2.3.4 EXCretion ............. i 61 2.3.4.1 Inhalation Exposure ................... 61 23.42 Oral EXposure ...............ouuuuuuuui 61 2.3.43 Dermal EXposure ................... 62 2.4 Mechanisms of Action ................. 62 2.5 RELEVANCE TO PUBLIC HEALTH ..............c.0ooooo 64 2.6 BIOMARKERS OF EXPOSURE AND EFFECT .............0oo 78 2.6.1 Biomarkers Used to Identify or Quantify Exposure to Hexachloroethane . . . ....... 79 2.6.2 Biomarkers Used to Characterize Effects Caused by Hexachloroethane ........... 79 2.7 INTERACTIONS WITH OTHER SUBSTANCES ............... 00 80 2.8 POPULATIONS THAT ARE UNUSUALLY SUSCEPTIBLE ..............\. 81 2.9 METHODS FOR REDUCING TOXIC EFFECTS ...........ooo 82 2.9.1 Reducing Peak Absorption Following EXposure .......................... 82 2.9.2 Reducing Body Burden ...................... 83 2.9.3 Interfering with the Mechanism of Action for Toxic Effects .................... 83 2.10 ADEQUACY OF THE DATABASE .........oooiin 84 2.10.1 Existing Information on Health Effects of Hexachloroethane ................... 84 2.10.2 Identification of Data Needs ........................ iii 85 2.10.3 On-going Studies ............... oii 95 3. CHEMICAL AND PHYSICAL INFORMATION .............. 00 97 3.1 CHEMICAL IDENTITY .........oo iii 97 3.2 PHYSICAL AND CHEMICAL PROPERTIES ...............0 0 97 4. PRODUCTION, IMPORT, USE, AND DISPOSAL .......... 0000 101 4.1 PRODUCTION ........ iii 101 4.2 IMPORT/EXPORT ........oiiniiiiii 103 43 USE. 103 HEXACHLOROETHANE xiii 5. POTENTIAL FOR HUMAN EXPOSURE ...... cies 105 5.1 OVERVIEW ott ee eee ee 105 52 RELEASES TO THE ENVIRONMENT .... eee 105 LR 0 BY | Epp EE 107 B07 WHEE +o invmume ns mmarss ida asndiat@uss ss smmanns cv smwulos rs nasnsss 109 5.0.3 SOM + tt 109 53 ENVIRONMENTAL FATE . oe 110 5.3.1 Transport and Partitioning ...............ooiinnnnnii 110 5.3.2 Transformation and Degradation ................c.oiiiniiiiiiinn. 111 B30 Al. iunuvssenmmuns camemmnssnrasdatts HERES 22 summn ws es vmns 111 BBY WWAIEE «vv vvvssmmmnnns cama ints i i ambsiessaansvans ss cmmmuss isn 111 5.3.2.3 Sediment and Soil .... oi 112 54 LEVELS MONITORED OR ESTIMATED IN THE ENVIRONMENT ............... 113 SA] AIT eee es 113 SAT WARIEE +0 tues snnm mnt es vsmusmss se sEasvsessnsnosssstsmavsss bosons ess 113 5.4.3 Sediment and Soil... o.oo 114 5.4.4 Other Environmental Media ....... cc. 114 55 GENERAL POPULATION AND OCCUPATIONAL EXPOSURE .................. 114 56 POPULATIONS WITH POTENTIALLY HIGH EXPOSURES ...................... 115 57 ADEQUACY OFTHE DATABASE ..... oes 115 5.7.1 Identification of Data Needs ........ oti iii 115 572 On-going Stdies .........coiirrriiiiiiii re 118 6. ANALYTICAL METHODS . «otitis 119 6.1 BIOLOGICAL MATERIALS titi ee 119 6.2 ENVIRONMENTAL SAMPLES . oie 120 6.3 ADEQUACY OFTHEDATABASE ..........ciiiiiiiiiiie ees 125 6.3.1 Identification of Data Needs . . ... ove 125 6.3.2 On-going SUES ........otitiii re 126 7. REGULATIONS AND ADVISORIES... ee 129 8 REFERENCES +s os mmmns vt suns sh samosas ss esawnnss smsmant st sdmansssssmannns 133 0. (TLJOSSARY . i tunings vanamans arama ssn ENE SAE A aaa as amen a a 147 APPENDICES A. MINIMAL RISK LEVEL WORKSHEETS .... ees A-1 B. USER'S GUIDE .. oii itt ttt im enssnsanssnssssnnantassassssssssssasssascrnnsvnnsss B-1 C. ACRONYMS, ABBREVIATIONS, AND SYMBOLS ............ooiiiinn C-1 HEXACHLOROETHANE XV 2-1. 2-2. 2-3. 5-1. LIST OF FIGURES Levels of Significant Exposure to Hexachloroethane - Inhalation ......................... 17 Levels of Significant Exposure to Hexachloroethane - Oral .................oonnnnn 36 Metabolism of Hexachloroethane . .......... c.count 60 . Existing Information on Health Effects of Hexachloroethane .........................o0n 86 Frequency of NPL Sites with Hexachloroethane Contamination ......................... 106 HEXACHLOROETHANE xvii LIST OF TABLES . Levels of Significant Exposure to Hexachloroethane - Inhalation ........o0suseesvamensase 12 . Levels of Significant Exposure to Hexachloroethane - O18] .. comms ss i BEE EYE Tm sn 29 . Levels of Significant Exposure to Hexachloroethane - Dermal ..oovvissiiimumusnssmomunss 51 . Genotoxicity of Hexachloroethane In Vitro .................ooooniirnnnnnrne ns 75 . Chemical Identity of Hexachloroethane .................ovvinnninernnneneeee sy 98 Physical and Chemical Properties of Hexachloroethane ...............oeiioiinnennnn.. 99 _ Facilities That Manufacture or Process Hexachloroethane ................ooovvveeeene 102 _ Releases to the Environment from Facilities That Manufacture or Process Hexachloroethane .. 108 . Analytical Methods for Determining Hexachloroethane in Biological Materials ............. 121 . Analytical Methods for Determining Hexachloroethane in Environmental Samples .......... 123 . Regulations and Guidelines Applicable to Hexachloroethane ................c.oooninnn 130 HEXACHLOROETHANE 1 1. PUBLIC HEALTH STATEMENT This statement was prepared to give you information about hexachloroethane and to emphasize the human health effects that may result from exposure to it. The Environmental Protection Agency (EPA) has identified 1,416 hazardous waste sites as the most serious in the nation. These sites make up the National Priorities List (NPL) and are the sites targeted for long-term federal clean-up activities. Hexachloroethane has been found in at least 45 of the sites on the NPL. However, the number of NPL sites evaluated for hexachloroethane is not known. As EPA evaluates more sites, the number of sites at which hexachloroethane is found may increase. This information is important because exposure to hexachloroethane may cause harmful health effects and because these sites are potential or actual sources of human exposure to hexachloroethane. When a substance is released from a large area, such as an industrial plant, or from a container, such as a drum or bottle, it enters the environment. This release does not always lead to exposure. You can be exposed to a substance only when you come in contact with it. You may be exposed by breathing, eating, or drinking substances containing it or by touching it. If you are exposed to a substance such as hexachloroethane, many factors will determine whether harmful health effects will occur and what the type and severity of those health effects will be. These factors include the dose (how much), the duration (how long), the route or pathway by which you are exposed (breathing, eating, drinking, or skin contact), the other chemicals to which you are exposed, and your individual characteristics such as age, sex, nutritional status, family traits, lifestyle, and state of health. HEXACHLOROETHANE 2 1. PUBLIC HEALTH STATEMENT 1.1 WHAT IS HEXACHLOROETHANE? Hexachloroethane is a colorless solid that gradually evaporates when it is exposed to air. This compound is also called perchloroethane, carbon hexachloride, and HCE. It is sold under the trade names Avlothane, Distokal, Distopan, and Distopin. In the United States, about half of the hexachloroethane is used by the military for smoke-producing devices. It is also sold as degassing pellets that are used to remove the air bubbles in melted aluminum. Hexachloroethane may be present as an ingredient in some fungicides, insecticides, lubricants, plastics, and cellulose. At one time, hexachloroethane was prescribed for deworming animals. Hexachloroethane does not occur naturally in the environment. It is made by adding chlorine to tetrachloroethylene. Hexachloroethane is no longer made in the United States, but it is formed as a by-product in the production of some chemicals. For example, it is a by-product in the high temperature synthesis of tetrachloroethylene from carbon tetrachloride. Some hexachloroethane can be formed by incinerators when materials containing chlorinated hydrocarbons are burned. Hexachloroethane itself does not easily catch fire. Some hexachloroethane can also be formed when chlorine reacts with carbon compounds in drinking water. Hexachloroethane vapors smell like camphor. You can begin to smell hexachloroethane in air when there are 150 parts present in a billion parts of air (ppb). You can smell it in water at 10 ppb. Neither a description of the taste nor the amount of hexachloroethane that gives a taste to water were found. For more information on the properties and uses of hexachloroethane, see Chapters 3, 4, and 5. 1.2. WHAT HAPPENS TO HEXACHLOROETHANE WHEN IT ENTERS THE ENVIRONMENT? Hexachloroethane is released to the air during military operations and training exercises when smoke-producing devices containing it are used. In a smoke pot or grenade, most of it is used up HEXACHLOROETHANE 1. PUBLIC HEALTH STATEMENT by the smoke-producing reaction. Only small amounts (5% or less) remain after the smoke has formed. However, these small amounts can collect in the atmosphere and in the soil. At one military training site, about 14,700 pounds of hexachloroethane were released to the air over a 2-year period. Hexachloroethane also enters the environment as part of the waste from companies that make or use it. Vapors can be released to the air during production, use, or transport. Solid wastes containing it are buried in landfills or burned. In landfills, it can dissolve in underground water because it does not bind strongly to soil. Once dissolved, it can reach rivers, lakes, streams, or well water. Hexachloroethane in the air does not break down to other compounds. It gradually escapes into the upper atmosphere. Some hexachloroethane that is in lakes or streams and surface soils will evaporate into the air. Some will be broken down by microscopic organisms. Microbes can break down hexachloroethane more easily without oxygen than with oxygen. That is why hexachloroethane will break down more quickly when it is buried in the soil or trapped in underground water than when it is near the surface. In one study, it took only 4 days for 99% of the hexachloroethane in soil to break down when oxygen was not present. It took 4 weeks when oxygen was present. Hexachloroethane does not appear to collect in plants or animals used for food. It has a slight tendency to build up in fish, but the fish break it down quickly, so the amount found in fish from polluted waters is very low. Rainbow trout from Lake Ontario had only 0.03 parts hexachloroethane per trillion (ppt) parts of fish. More information on what happens to hexachloroethane in the environment is in Chapters 4 and 5. HEXACHLOROETHANE 4 1. PUBLIC HEALTH STATEMENT 1.3 HOW MIGHT | BE EXPOSED TO HEXACHLOROETHANE? You can be exposed to hexachloroethane from the air. Background levels in air range from 5 to 7 ppt. Larger amounts may be found near military installations where smoke pots and grenades that contain hexachloroethane are used during training. When a smoke pot or grenade is used, the heat will cause other chemicals to be formed, including tetrachloroethylene, carbon tetrachleride, phosgene, and hexachlorobenzene. These chemicals can also be toxic. Higher than average amounts can occur near aluminum smelters that use hexachloroethane as a degassing agent. Incinerators that burn industrial wastes containing chlorine can release hexachloroethane to the air. [f you live near a hazardous waste site, you might be exposed to hexachloroethane by breathing or by drinking contaminated water. Private wells within one mile of a hazardous waste site contained 4.6 ppb hexachloroethane. Children who play in soil near a waste site that contains hexachloroethane could be exposed if they put soil or soiled fingers into their mouths. You are not likely to be exposed to hexachloroethane from your food. However, you might be exposed if you use insecticides, fungicides, or plastics that contain this chemical. You may also be exposed to small amounts of this chemical from your drinking water if chlorine is used to kill germs. Hexachloroethane has occasionally been reported in drinking water at concentrations of 0.03-4.3 ppb in some locations in the United States. [f you work in an industry that uses hexachloroethane, such as aluminum smelting, or a chemical plant, you could be exposed by breathing it or touching it. About 8,500 people in the United States are exposed to hexachloroethane at work. People who work with smoke-producing devices that contain hexachloroethane are exposed to it in the smoke. They can contact it through smoke particles on plants and in the soil. More information on how you can be exposed to hexachloroethane is in Chapter 5. HEXACHLOROETHANE 5 1. PUBLIC HEALTH STATEMENT 1.4 HOW CAN HEXACHLOROETHANE ENTER AND LEAVE MY BODY? Hexachloroethane can enter your body through your lungs if you breathe its vapors. Of the amount that enters your lungs, only a small fraction of the hexachloroethane will enter your bloodstream and ultimately your body tissues. It can enter your body if you eat or drink something contaminated with it. Based on studies in animals, about half of the hexachloroethane you eat will get into your bloodstream. Very little will enter your body if you get it on your skin. The hexachloroethane that enters your bloodstream will go to your liver where it is turned into other compounds. Some of these compounds are harmful and will affect your health in almost the same way hexachloroethane does. If you are exposed to carbon tetrachloride, your liver can make hexachloroethane from it. When hexachloroethane gets into your body, some is temporarily stored in your body fat. Most of it leaves your body in 1 or 2 days in the air you breathe out, in your urine, and in your feces. More information on how hexachloroethane enters and leaves your body is in Chapter 2. 1.5 HOW CAN HEXACHLOROETHANE AFFECT MY HEALTH? Mild skin irritation has been reported by workers at a munitions factory who were exposed to low levels of hexachloroethane. The workers were wearing protective clothing that greatly reduced exposure. No other information is available concerning health effects in people exposed to hexachloroethane. However, results of animal studies can be used to show how it can affect your health. Based on the animal data, hexachloroethane in the air can irritate your nose and lungs and cause some buildup of mucus in your nose, much like an allergy. It can also irritate your eyes and make them tear. If you are in an area that has a lot of hexachloroethane vapor, your facial muscles may twitch or you may have difficulty moving. These effects have been observed in animals during exposure HEXACHLOROETHANE 6 1. PUBLIC HEALTH STATEMENT at levels far greater than those found in industrial use of hexachloroethane or those which would be expected in areas near a hazardous waste site. Hexachloroethane is not a highly toxic substance. If you are exposed to a large amount for a long time, some of your liver cells could be destroyed and fat could build up in your liver. There is also a slight chance that your kidneys could be damaged. No results from animal studies suggest that hexachloroethane would make it hard for you to become pregnant or that it would hurt your baby while you are pregnant. However, animal studies that have looked at the effects of hexachloroethane during pregnancy are limited. Liver tumors developed in mice that were orally exposed to hexachloroethane for their whole lifetime. Tumors of this kind are common in mice. Hexachloroethane will not necessarily have the same effect on people. Male rats that were exposed to hexachloroethane for their lifetime developed kidney tumors. This type of tumor is not found in people, so it is unlikely that exposure to hexachloroethane would cause you to develop cancer of the kidney. The Department of Health and Human Services has determined that hexachloroethane may reasonably be anticipated to be a carcinogen (can cause cancer). The International Agency for Research on Cancer (IARC) has determined that hexachloroethane is not classifiable as to its carcinogenicity in people. EPA has determined that hexachloroethane is a possible human carcinogen. More information on the health effects from hexachloroethane exposure is in Chapter 2. 1.6 IS THERE A MEDICAL TEST TO DETERMINE WHETHER | HAVE BEEN EXPOSED TO HEXACHLOROETHANE? Samples of your blood, urine, or feces can be tested to see if you were exposed to hexachloroethane. The tests are not routinely available at most doctors’ offices, but your doctor can collect blood, urine, or fecal samples and send them to a special laboratory for testing. These tests are useful only if you were exposed 24-48 hours before you saw the doctor. Your body changes hexachloroethane into the same compounds that it makes from other chemicals like HEXACHLOROETHANE 7 1. PUBLIC HEALTH STATEMENT tetrachloroethylene or pentachloroethane. Your body can also make hexachloroethane from carbon tetrachloride. Therefore, if a laboratory finds hexachloroethane in your body blood or excretions, your doctor will ask you if you were exposed to carbon tetrachloride. More information on medical tests that can be used to determine if you have been exposed to hexachloroethane is in Chapters 2 and 6. 1.7 WHAT RECOMMENDATIONS HAS THE FEDERAL GOVERNMENT MADE TO PROTECT HUMAN HEALTH? The federal government is concerned about the amount of hexachloroethane that you are exposed to in the environment. The government has established standards and guidelines to prevent you from being overexposed. The Occupational Safety and Health Administration (OSHA) has set a limit of 1 part per million (ppm) for the hexachloroethane in workplace air over an 8-hour workday. The National Institute for Occupational Safety and Health (NIOSH) considers hexachloroethane as a potential occupational carcinogen (can cause cancer) and recommends 1 ppm in air as a tolerance value. The EPA recommends that children not drink water with more than 5 ppm hexachloroethane for more than 10 days or more than 100 ppb for any longer than 7 years. Adults should not drink water with more than 450 ppb any longer than 7 years. EPA suggests that water consumed over a lifetime contain no more than 1 ppb hexachloroethane. Industrial releases of more than 100 pounds of hexachloroethane into the environment must be reported to EPA. More information on government regulations for hexachloroethane is in Chapter 7. HEXACHLOROETHANE 1. PUBLIC HEALTH STATEMENT 1.8 WHERE CAN | GET MORE INFORMATION? If you have any more questions or concerns, please contact your community or state health or environmental quality department or Agency for Toxic Substances and Disease Registry Division of Toxicology 1600 Clifton Road NE, Mailstop E-29 Atlanta, Georgia 30333 (404) 639-6000 This agency can also provide you with information on the location of occupational and environmental health clinics. These clinics specialize in the recognition, evaluation, and treatment of illness resulting from exposure to hazardous substances. HEXACHLOROETHANE oO 2. HEALTH EFFECTS 2.1 INTRODUCTION The primary purpose of this chapter is to provide public health officials, physicians, toxicologists, and other interested individuals and groups with an overall perspective on the toxicology of hexachloroethane. It contains descriptions and evaluations of toxicological studies and epidemiological investigations and provides conclusions, where possible, on the relevance of toxicity and toxicokinetic data to public health. A glossary and list of acronyms, abbreviations, and symbols can be found at the end of this profile. 2.2 DISCUSSION OF HEALTH EFFECTS BY ROUTE OF EXPOSURE To help public health professionals and others address the needs of persons living or working near hazardous waste sites, the information in this section is organized first by route of exposure — inhalation, oral, and dermal; and then by health effect — death, systemic, immunological, neurological, reproductive, developmental, genotoxic, and carcinogenic effects. These data are discussed in terms of three exposure periods — acute (14 days or less), intermediate (15-364 days), and chronic (365 days or more). Levels of significant exposure for each route and duration are presented in tables and illustrated in figures. The points in the figures showing no-observed-adverse-effect levels (NOAELs) or lowest-observed- adverse-effect levels (LOAELS) reflect the actual doses (levels of exposure) used in the studies. LOAELS have been classified into "less serious" or "serious" effects. "Serious" effects are those that evoke failure in a biological system and can lead to morbidity or mortality (e.g., acute respiratory distress or death). "Less serious" effects are those that are not expected to cause significant dysfunction or death, or those whose significance to the organism is not entirely clear. ATSDR acknowledges that a considerable amount of judgment may be required in establishing whether an end point should be classified as a NOAEL, "less serious" LOAEL, or "serious" LOAEL, and that in some cases, there will be insufficient data to decide whether the effect is indicative of significant dysfunction. However, the Agency has established guidelines and policies that are used to classify these end points. ATSDR believes that there is sufficient merit in this approach to warrant an attempt at distinguishing between "less serious” and "serious" effects. The distinction between "less serious" effects and "serious" effects is considered to be HEXACHLOROETHANE 10 2. HEALTH EFFECTS important because it helps the users of the profiles to identify levels of exposure at which major health effects start to appear. LOAELs or NOAELSs should also help in determining whether or not the effects vary with dose and/or duration, and place into perspective the possible significance of these effects to human health. The significance of the exposure levels shown in the Levels of Significant Exposure (LSE) tables and figures may differ depending on the user's perspective. Public health officials and others concerned with appropriate actions to take at hazardous waste sites may want information on levels of exposure associated with more subtle effects in humans or animals or exposure levels below which no adverse effects have been observed. Estimates of levels posing minimal risk to humans (Minimal Risk Levels or MRLs) may be of interest to health professionals and citizens alike. Levels of exposure associated with carcinogenic effects (Cancer Effect Levels, CELSs) of hexachloroethane are indicated in Table 2-2 and Figure 2-2. Because cancer effects could occur at lower exposure levels, Figure 2-2 also shows a range for the upper bound of estimated excess risks, ranging from a risk of 1 in 10,000 to 1 in 10,000,000 (10 to 107), as developed by EPA. Estimates of exposure levels posing minimal risk to humans (Minimal Risk Levels or MRLs) have been made for hexachloroethane. An MRL is defined as an estimate of daily human exposure to a substance that is likely to be without an appreciable risk of adverse effects (noncarcinogenic) over a specified duration of exposure. MRLs are derived when reliable and sufficient data exist to identify the target organ(s) of effect or the most sensitive health effect(s) for a specific duration within a given route of exposure. MRLs are based on noncancerous health effects only and do not consider carcinogenic effects. MRLs can be derived for acute, intermediate, and chronic duration exposures for inhalation and oral routes. Appropriate methodology does not exist to develop MRLs for dermal exposure. Although methods have been established to derive these levels (Barnes and Dourson 1988; EPA 1990e), uncertainties are associated with these techniques. Furthermore, ATSDR acknowledges additional uncertainties inherent in the application of the procedures to derive less than lifetime MRLs. As an example, acute inhalation MRLs may not be protective for health effects that are delayed in development or are acquired following repeated acute insults, such as hypersensitivity reactions, asthma, or chronic bronchitis. As these kinds of health effects data become available and methods to assess levels of significant human exposure improve, these MRLs will be revised. HEXACHLOROETHANE 11 2. HEALTH EFFECTS A User's Guide has been provided at the end of this profile (see Appendix A). This guide should aid in the interpretation of the tables and figures for Levels of Significant Exposure and the MRLs. 2.21 Inhalation Exposure Hexachloroethane is a solid that sublimes at ambient air temperatures. At 20°C the saturated vapor concentration is 670-700 ppm (Weeks et al. 1979); thus, there is a limitation on the vapor concentration that can be used in studies using the inhalation route of exposure. In circumstances where the saturation threshold is exceeded, microcrystalline hexachloroethane forms in the atmosphere and is inhaled by the exposed animals along with the volatilized hexachloroethane. 2.2.1.1 Death No studies were located regarding death in humans after inhalation exposure to hexachloroethane. Rats were exposed to vapor concentrations of either 260 or 5,900 ppm hexachloroethane for 8 hours (Weeks et al. 1979). The 5,900 ppm vapor concentration was generated at 50°C and crystallized as it entered the exposure chamber. At the higher concentration the exposed animals showed signs of distress (staggering gait) during exposure, and 2 of 6 were dead at the end of 8 hours. No animals died at the lower exposure concentration. Following 6 weeks of inhalation exposure to 15-260 ppm, no deaths in quail were reported; however, 2 of 50 rats, 4 of 10 guinea pigs, and 1 of 4 dogs died at the 260 ppm concentration (Weeks et al. 1979). Based on clinical signs, the dogs seemed to be particularly sensitive to hexachloroethane exposure. The animals developed tremors and ataxia and closed their eyes. The one dog that died experienced convulsions before death. The rats and guinea pigs that succumbed to exposure died during weeks 4 or 5 and, thus, appear to be less sensitive. The quail were the most resistant to death following hexachloroethane exposure. All identified LOAEL values for lethality in each species and duration category are recorded in Table 2-1 and plotted in Figure 2-1. These values indicate that hexachloroethane is lethal to animals exposed intermittently to 260 ppm for 6 weeks; however, no deaths occurred in animals acutely exposed for 8 hours to the same concentration. Concentrations of 48 ppm and lower were not lethal in rats, guinea pigs, dogs, or quail. TABLE 2-1. Levels of Significant Exposure to Hexachloroethane - Inhalation Key a Exposure LOAEL (effect) to Species duration/ NOAEL Serious figure (strain) frequency System (ppm) (ppm) Reference ACUTE EXPOSURE Death 1 Rat 8 hr 5900 M (2/6 rats died) Weeks et al. 1979 (Sprague- Dawley) Systemic 2 Rat 8 hr Resp 260 M 5900 M (interstitial pneumonitis Weeks et al. 1979 (Sprague- in 2/4 survivors) Dawley) Cardio 5900 M Gastro 5900 M Musc/skel 5900 M Hepatic 5900 M Renal 5900 M Endocr 5900 M Derm 5900 M Bd Wt 260 M 5900 M (reduced body weight gain, quantitative data not provided) Neurological 3 Rat 6 hr 260 M 5900 M (staggered gait Weeks et al. 1979 (Sprague- in 1/6 rats) Dawley) 4 Rat 11d 48b F 260 F (tremors) Weeks et al. 1979 (Sprague- Gd 6-16 Dawley) 6hr/d S103443 H1IV3H ¢ 3NVHLIOHOTHOVX3H cl TABLE 2-1. Levels of Significant Exposure to Hexachloroethane - Inhalation (continued) Key * Exposure LOAEL (effect) to Species duration/ NOAEL Less serious Serious figure (strain) frequency System (ppm) (ppm) (ppm) Reference Reproductive 5 Rat 11d 260 F Weeks et al. 1979 (Sprague- Gd 6-16 Dawley) 6hr/d Developmental 6 Rat 11d 260 Weeks et al. 1979 (Sprague- Gd 6-16 Dawley) 6hr/d INTERMEDIATE EXPOSURE Death 7 Gn pig 6 wk 260 M (4/10 guinea pigs died) Weeks et al. 1979 (Hartley) 5d/wk 6hr/d 8 Dog 6 wk 260 M (1/4 dogs died) Weeks et al. 1979 (Beagle) 5d/wk 6hr/d S103443 H1IV3H 2 INVHLIOHOTHOVX3H 138 TABLE 2-1. Levels of Significant Exposure to Hexachloroethane - Inhalation (continued) Key e Exposure LOAEL (effect) to Species duration/ NOAEL Less serious Serious figure (strain) frequency System (ppm) (ppm) (ppm) Reference Systamic 9 Rat 6 wk Resp 48 260 (reduced resistance to Weeks et al. 1979 (Sprague- 5d/wk endemic mycoplasia Dawley) 6hr/d infection; mucopurulent exudate in the nasal cavities; lymphoid hyperplasia in the trachea and pneumonitis) Cardio 260 Gastro 260 Musc/skel 260 Hepatic 260 Renal 260 Endocr 260 Derm 260 Ocular 48 260 (irritation) Bd Wt 48 260 M (reduced body weight, quantitative data not provided) 10 Rat 6 wk Resp 260 Weeks et al. 1979 (Sprague- 5d/wk Dawley) 6hr/d Hepatic 260 Renal 260 Bd Wt 48 260 M (mean body weights decreased 11% in older animals) S103443 H1TV3H 2 INVHLIOHOTHOVX3H vi TABLE 2-1. Levels of Significant Exposure to Hexachloroethane - Inhalation (continued) Key * Exposure LOAEL (effect) to Species duration/ NOAEL Less serious Serlous figure (strain) frequency System (ppm) (ppm) (ppm) Reference 11 Gn pig 6 wk Resp 260 M Weeks et al. 1979 (Hartley) 5d/wk 6hr/d Cardio 260 M Gastro 260 M Musc/skel 260 M Hepatic 260 M Renal 260 M Derm 260 M Ocular 260 M Bd Wt 48 M 260 M (reduced body weight gain, quantitative data not provided) 12 Dog 6 wk Resp 260 M Weeks et al. 1979 (Beagle) 5d/wk 6hr/d Cardio 260 M Hemato 260 M Musc/skel 260 M Hepatic 260 M Renal 260 M Endocr 260 M Derm 260 M Ocular 48 M 260 M (irritation) Bd Wt 260 M Neurological 13 Rat 6 wk 260 M Weeks et al. 1979 (Sprague- 5d/wk Dawley) 6hr/d S103443 H1V3H ¢ INVHLIOHOTHOVX3IH Sl TABLE 2-1. Levels of Significant Exposure to Hexachloroethane - Inhalation (continued) Key * Exposure LOAEL (effect) to Species duration/ NOAEL Less serious Serious figure (strain) frequency System (ppm) (ppm) (ppm) Reference 14 Rat 6 wk 48 c 260 (tremors) Weeks et al. 1979 (Sprague- 5d/wk Dawley) 6hr/d 15 Dog 6 wk 48 M 260 M (tremors; ataxia; Weeks et al. 1979 (Beagle) 5d/wk fasciculations; severe head 6hr/d bobbing) *The number corresponds to entries in Figure 2-1. ®Used to derive an acute-duration inhalation minimal risk level (MRL) of 6 ppm. The NOAEL was converted to a Human Equivalent Concentration (HEC) of 181 ppm by multiplying by (0.22 m*/day/0.204 kg), the reference value for Sprague-Dawley rats (EPA 1988a), and dividing by (20 m°*/day/70kg), the reference value for humans (EPA 1988a). The HEC was divided by an uncertainty factor of 30 (3 to extrapolate from animals to humans, and 10 for human variability). “Used to derive an intermediate-duration inhalation MRL of 6 ppm. The NOAEL was converted to a Human Equivalent Concentration (HEC) of 174 ppm by multiplying by (0.245 m*/day/0.236 kg), the reference values for Sprague-Dawley rats (EPA 1988a), and divided by (20 m*/day/70kg), the reference values for humans (EPA 1988a). The HEC was divided by an uncertainty factor of 30 (3 to extrapolate from animals to humans, and 10 for human variability). Bd Wt = body weight; Cardio = cardiovascular; d = day(s); Derm = dermal; Endocr = endocrine; F = female; Gastro = gastrointestinal; Gd = gestation day(s); Gn pig = guinea pig; Hemato = hematological; hr = hour(s); LOAEL = lowest-observed-adverse-effect level; M = male; Musc/skel = musculoskeletal; NOAEL = no-observed-adverse-effect level; Resp = respiratory; wk = week(s) S103443 H1TV3H 2 IANVHLIOHOTHOVXIH 91 Figure 2-1. Levels of Significant Exposure to Hexachlorethane - Inhalation INVHLIOHOTHOVX3H S103443 H1TV3H ¢ Acute (<14 days) Systemic \ N $ @ x2 AEN 2 x 5 $$ & fF ) ) & > XS ¥ & © . & \ © S > (ppm) ¢ & FF F&F 5 FQ \© NN 8 O > Q o << 3 & § 10.000 2 _% NRX 9 Q ~ TQ ®e O oO OO O oO oO OO Oo Oo ® 1r 2r 2r 2r 2r 2r 2r 2r 2r 2r 3r 1,000 [— O Oo O ® O O 100 — 2r 2r ar ar 5r br O 2 i 10 — | wv 1.0— 0.1 Key 801 The number next to each ¢ Rat . ) point corresponds to 0.001 — : @ LOAEL for serious effects (animals) entries in Table 2-1. ’ g Guinea pig (P LOAEL for less serious effects (animals) 4 Dog OO NOAEL (animals) ' Minimal risk level for effects 0.0001 — , other than cancer / Ll Figure 2-1. Levels of Significant Exposure to Hexachloroethane - Inhalation (continued) Intermediate (15-364 days) Systemic N $C DAP Q N° EN &F o° & > 0 & 2 S° F i © 5 &° NL (ppm) ° © OS SS © » & < F Q Fo © > ¢ & & 9 3 ? & FPF RX & & & > $O > Q <& oY OTR Vs I «9 0 Q 1,000 — 10r 12d 11g gor 12d 1g 9 11g 9 11g 9r or 124 1g or 11g ® 00 000003 00000 B00 303000 @ bi or CQO¢ 2OR0% 12d 10r 12d 10r 12d 12d @ 9 12d 10r 12d 13r 14r 15d 100 — 12d 1or 14r 0 O 00 OO or ar or 11g 15d | I — I 10 3 Key 1 = The number next to each } } point corresponds to r Rat @ LOAEL for serious effects (animals) entries in Table 2-1. g Guinea pig (DP LOAEL for less serious effects (animals) 4 Dog (O NOAEL (animals) | Minimal risk level for effects , other than cancer Vv S103443 H1V3H ¢ INVHLIOHOTHOVX3H 81 HEXACHLOROETHANE 19 2. HEALTH EFFECTS 2.2.1.2 Systemic Effects The highest NOAEL values and all LOAEL values from each reliable study for systemic effects in each species and duration category are recorded in Table 2-1 and plotted in Figure 2-1. Respiratory Effects. Pulmonary function tests (vital capacity, forced expiratory volume at 1 second) were in the normal range in 11 workers occupationally exposed to hexachloroethane at 0.5-2.1 ppm while wearing protective equipment including compressed-air-fed visors or full-facepiece masks with combination filters (Selden et al. 1994). The testing was compieted 5 weeks after production at a smoke munitions plant resumed following a 5-week break. Plasma hexachloroethane levels were 0.08 + 0.14 pg/L before production resumed and 7.3 + 6.04 pg/L 5 weeks later indicating that despite protective equipment, low-level exposure occurred (Selden et al. 1993). Mild skin and mucous membrane irritation were reported in the exposed group, suggesting that exposure may have been through either the inhalation or dermal routes of exposure. Acute exposure of rats to 5,900 ppm hexachloroethane for 8 hours caused interstitial pulmonary pneumonitis (Weeks et al. 1979). At this exposure concentration there were hexachloroethane particles present in the exposure chamber that were inhaled and probably contributed to the lung irritation. Changes in lung histopathology were noted when the animals were sacrificed after a 14-day recovery period. There were no changes in relative lung weights or tissue histopathology in animals that were exposed to 260 ppm for the same time period. When pregnant female rats were exposed to 0, 15, 48, or 260 ppm hexachloroethane on gestation days 6-16, 85% of the animals in the 48-ppm dose group displayed nasal exudate, and all animals in the 260-ppm dose group were affected. There was an endemic mycoplasma infection in the colony of rats used in the Weeks et al. (1979) study. Therefore, it is not clear if the increase in nasal exudate observed at 48 ppm in the teratology study, but not at 48 ppm in the 6-week study (discussed below), was truly related to exposure. In rats exposed to 260 ppm hexachloroethane for 6 weeks, there was a significant decrease in oxygen consumption as compared to the controls (Weeks et al. 1979). Oxygen consumption was determined by measuring carbon dioxide exhaled by rats placed in a water-sealed chamber for 15 minutes. The authors hypothesized that the decrease in oxygen consumption could have been a normal response to inhalation of a respiratory tract irritant. There were no significant changes in lung weights, but there was an increase in HEXACHLOROETHANE 20 2. HEALTH EFFECTS mycoplasma lesions of the nasal turbinates, trachea, and lungs; lymphoid hyperplasia of the trachea; and pneumonitis of the bronchi when the animals were sacrificed after the 6-week exposure period. These changes were not seen in the animals exposed to 15 or 48 ppm or in rats exposed to 260 ppm and sacrificed after a 12-week recovery period. The authors hypothesized that the respiratory tract lesions were the result of hexachloroethane potentiation of an endemic mycoplasma infection rather than systemic effects from inhalation exposure to hexachloroethane. The infection could be the result of lowered host resistance due to either compromised immune defenses or a weakened mucosal barrier along the respiratory epithelium. In older rats (12-14 weeks), there was a significant increase in relative lung weights as compared to controls following 6 weeks of exposure to 260 ppm hexachloroethane. Oxygen consumption was not measured in these animals, and it is not clear if the tissues were examined histologically (Weeks et al. 1979). In dogs, there were no significant changes in pulmonary function with exposure to 15-260 ppm hexachloroethane for 6 weeks (Weeks et al. 1979). Intrapleural pressure, transpulmonary pressure, air flow, and tidal volume were measured to obtain scores for compliance and resistance. When the animals were sacrificed at either 6 weeks or after a 12-week recovery period, there were no histopathological changes observed in the lungs. There were also no apparent effects on the respiratory system in guinea pigs from exposure to 15-260 ppm hexachloroethane. Exposure of quail to 260 ppm was associated with increased mucus in the nasal turbinates in 2 of the 10 animals, but this increased mucus did not appear to be associated with a respiratory infection. These changes were considered to be the direct effect of hexachloroethane on the epithelium of the nasal cavity and are discussed in Section 2.2.3.2. Exposure to hexachloroethane vapors can cause irritation to the respiratory system. Acute exposure to 260 ppm hexachloroethane had no apparent effect on the lungs and air passages in rats, but acute exposure to a concentration where particulate hexachloroethane was present in the atmosphere caused lung irritation (Weeks et al. 1979). On the other hand, intermediate-duration exposure to 260 ppm hexachloroethane appeared to cause some irritation of the respiratory epithelium, which may have increased susceptibility to respiratory infection. When exposure ceased, the animals recovered, so there were no histopathological indications of tissue damage after a 12-week recovery period. Lesions of the nasal passages, trachea, and bronchi; increased mycoplasma infections; mucus in the nasal cavities; and decreased oxygen HEXACHLOROETHANE 21 2. HEALTH EFFECTS consumption were indicators of respiratory tract irritation from repeated episodes of hexachloroethane exposure. Cardiovascular Effects. No studies were located regarding cardiovascular effects in humans after inhalation exposure to hexachloroethane. There were no histopathological changes in the heart for rats, guinea pigs, dogs, or quail that were exposed to concentrations of 0, 260, or 5,900 ppm hexachloroethane for 8 hours or to 0, 15, 48, or 260 ppm hexachloroethane 6 hours/day, 5 days/week for 6 weeks (Weeks et al. 1979). Gastrointestinal Effects. No studies were located regarding gastrointestinal effects in humans after inhalation exposure to hexachloroethane. There were no histopathological changes in the stomach, small intestines, or large intestines for rats, guinea pigs, dogs, or quail that were exposed to concentrations of 0, 260, or 5,900 ppm hexachloroethane for 8 hours or to 0, 15, 48, or 260 ppm hexachloroethane 6 hours/day, 5 days/week for 6 weeks (Weeks et al. 1979). Hematological Effects. Routine blood parameters (hemoglobin, erythrocyte, leukocyte and thrombocyte levels) measured in 11 hexachloroethane workers did not differ from those of the controls (Selden et al. 1994). Plasma hexachloroethane levels in these workers, who wore protective equipment, were 7.3 + 6.04 pg/L at the time of the hematological analysis and 0.08 + 0.14 ng/L before production resumed (Selden et al. 1993). Mild skin and mucous membrane irritation were reported in the exposed group, suggesting that exposure may have been through either the inhalation or dermal routes of exposure. There were no effects on the red blood cell counts of dogs exposed to 0, 15, 48, or 260 ppm hexachloroethane for 6 weeks (Weeks et al. 1979). Although other hematological parameters were apparently determined, the red cell count was the only parameter that was specified. Accordingly, it is not possible to speculate whether inhalation exposure to hexachloroethane has any effect on other hematological parameters. HEXACHLOROETHANE ’ 22 2. HEALTH EFFECTS Musculoskeletal Effects. No studies were located regarding musculoskeletal effects in humans after inhalation exposure to hexachloroethane. There were no treatment-related gross or histopathological lesions of the skeletal muscle or bone in rats, guinea pigs, dogs, or quail exposed to 0, 15, 48, or 260 ppm hexachloroethane 6 hours/day, 5 days/week for 6 weeks (Weeks et al. 1979). Hepatic Effects. Liver function tests (serum bilirubin, alkaline phosphatase, aspartate aminotransferase, alanine aminotransferase, gamma-glutamyl transferase) completed in 11 hexachloroethane workers were within the normal range (Selden et al. 1994). Plasma hexachloroethane levels in these workers, who wore protective equipment, were 7.3 + 6.04 ug/L at the time of the tests (Selden et al. 1993). Mild skin and mucous membrane irritation were reported in the exposed group, suggesting that exposure may have been through either the inhalation or dermal routes of exposure. A single 8-hour exposure of rats to 260 ppm hexachloroethane had no effect on relative liver weight or tissue histopathology (Weeks et al. 1979). A single 8-hour exposure to 5,900 ppm did not cause histopathological changes. Organ weights were not determined for the higher exposure concentration. The relative liver weight was significantly increased (p value not given) in guinea pigs and rats, but not dogs or quail, that were exposed to 260 ppm 6 hours/day, 5 days/week for 6 weeks (Weeks et al. 1979). Since the increase in liver weight was not accompanied by any histological abnormalities, it is classified as a NOAEL rather than a LOAEL in Table 2-1 and Figure 2-1. There were no changes in liver weights or histopathology in any species exposed to concentrations of 15 or 48 ppm for 6 weeks. Renal Effects. Renal function tests (serum creatinine and urate, urinary hemoglobin, protein and glucose) completed in 11 hexachloroethane workers were within the normal range (Selden et al. 1994). Plasma hexachloroethane levels in these workers, who wore protective equipment, were 7.3 + 6.04 pg/L at the time of the tests (Selden et al. 1993). Mild skin and mucous membrane irritation were reported in the exposed group, suggesting that exposure may have been through either the inhalation or dermal routes of exposure. HEXACHLOROETHANE 23 2. HEALTH EFFECTS A single exposure of rats to 260 ppm hexachloroethane had no effect on relative kidney weight or tissue histopathology (Weeks et al. 1979). A single exposure to 5,900 ppm did not cause histopathological changes. Organ weights were not determined for the higher exposure concentration. The relative kidney weight was significantly increased (p value not stated) in male rats, but not female rats, guinea pigs, dogs, or quail, that were exposed to 260 ppm 6 hours/day, 5 days/week for 6 weeks (Weeks et al. 1979). Since the increase in kidney weight was not accompanied by any histological abnormalities, it is classified as a NOAEL rather than a LOAEL in Table 2-1 and Figure 2-1. There were no changes in kidney weights or histopathology in any species exposed to 15 or 48 ppm hexachloroethane for 6 weeks. Endocrine Effects. No studies were located regarding endocrine effects in humans after inhalation exposure to hexachloroethane. There were no histopathological changes in the pancreas or adrenal glands of rats exposed to concentrations of 0, 260, or 5,900 ppm hexachloroethane for 8 hours, or in the pancreas or adrenal glands of rats, guinea pigs, dogs, or quail exposed to 0, 15, 48, or 260 ppm hexachloroethane 6 hours/day, 5 days/week for 6 weeks (Weeks et al. 1979). Dermal Effects. Hexachloroethane exposed workers reported a slightly higher prevalence of dry skin and dry mucous membranes as well as itching and other skin problems than the unexposed controls (Selden et al. 1994). Clinical examinations of the 11 exposed workers did not reveal signs of abnormal dermatological or mucous membrane status. Plasma hexachloroethane levels in these workers, who wore protective equipment, were 7.3 + 6.04 ug/L at the time of the examinations (Selden et al. 1993). The investigators indicate that the dermal effects may also have been a result of a local trauma effect of the protective equipment. Ocular Effects. No studies were located regarding ocular effects in humans after inhalation exposure to hexachloroethane. Dogs that were exposed to 260 ppm hexachloroethane for 6 hours per day, 5 days per week, kept their eyes closed during each exposure (Weeks et al. 1979). Since this effect occurred throughout the 6-week study, it can be regarded as an acute effect that was most likely the result of vapor contact with the eye. In HEXACHLOROETHANE 24 2. HEALTH EFFECTS rats, a red exudate appeared about the eyes starting at week 4. This may have been a systemic effect. There were no reported effects on the eyes of guinea pigs or quail during 6 weeks of exposure to hexachloroethane. Body Weight Effects. Rats exposed to a concentration of 5,900 ppm hexachloroethane for 8 hours had a decreased weight gain over the 14-day, postexposure observation period when compared to controls (Weeks et al. 1979). There were no differences in the weight gain for animals exposed to 260 ppm under the same conditions. Guinea pigs and male rats had decreased weight gains starting at week 2 or 3 of an intermittent 6-week exposure to 260 ppm hexachloroethane, but there were no effects on dogs or quail (Weeks et al. 1979). Intermittent exposure to 15 or 48 ppm hexachloroethane for 6 weeks had no effect on weight gain in rats, dogs, guinea pigs, or quail. 2.2.1.3 Immunological and Lymphoreticular Effects No studies were located regarding immunological or lymphoreticular effects in humans after inhalation exposure to hexachloroethane. There were no treatment-related gross or histopathological lesions of the thymus and spleen and no changes in spleen weight in rats that were exposed to 260 or 5,900 ppm hexachloroethane for 8 hours, nor were there any effects on thymus and spleen histopathology in rats, guinea pigs, dogs, and quail that were exposed to 260 ppm 6 hours/day, 5 days/week for 6 weeks (Weeks et al. 1979). The relative spleen weight was significantly higher (p value not stated) than that for the controls in young male rats but was not affected in older male rats or any of the other species evaluated. No effects were seen in the 15 and 48 ppm dose groups. There was an increased incidence of a mycoplasma respiratory tract infection in rats exposed to 260 ppm hexachloroethane for 6 weeks but not in rats exposed to lower doses or in other species. This could indicate compromised immune function or a weakened mucosal barrier along the respiratory epithelium. There were no studies identified that evaluated a wide range of immunological parameters. Therefore, there are no reliable LOAELs or NOAELSs for this end point. Increases in spleen weights are not classified as LOAELS since they were not accompanied by histopathological changes. HEXACHLOROETHANE 25 2. HEALTH EFFECTS 2.2.1.4 Neurological Effects No studies were located regarding neurological effects in humans after inhalation exposure to hexachloroethane. Acute 8-hour exposures to 5,900 ppm, but not 260 ppm, resulted in a staggering gait in one of six rats (Weeks et al. 1979). Tremors were also noted in pregnant rats exposed 6 hours per day to 260 ppm starting on the 6th day of an 11-day exposure period but not in animals exposed to 15 or 48 ppm (Weeks et al. 1979). Based on the NOAEL for neurological effects, an acute inhalation MRL of 6 ppm was calculated, as described in the footnote in Table 2-1. When male rats were exposed to concentrations of 0, 15, 48, or 260 ppm hexachloroethane 6 hours/day, 5 days/week for 6 weeks, foot shock avoidance behavior and spontaneous motor activity were not different from controls when measured at 1 day, 3 weeks, or 6 weeks (Weeks et al. 1979). However, a group of male and female rats exposed to 260 ppm experienced tremors beginning at 4 weeks and persisting for the remainder of the 6-week exposure period. Recovery was evident during the 12-week post-exposure period (Weeks et al. 1978). Tremors were not observed in rats exposed at 48 ppm. Based on the intermediate-duration NOAEL of 48 ppm for neurological effects, an intermediate inhalation MRL of 6 ppm was calculated, as described in the footnote in Table 2-1. Dogs were apparently quite sensitive to neurological effects during hexachloroethane exposure (Weeks et al. 1979). The animals displayed tremors, ataxia, head bobbing, and fasciculation of the facial muscles with a 260 ppm exposure. Symptoms disappeared in the interval between exposures but returned intermittently over the 6-week exposure period. There were no differences in serum cholinesterase activity between control and exposed animals. Apparently, the levels of the neurotransmitter acetylcholine were not affected by hexachloroethane. There were no neurological responses in guinea pigs or quail with a 260-ppm exposure, and none of the species evaluated showed any overt neurological responses with an intermittent 6-week exposure at 15 or 48 ppm. The highest NOAEL values and all LOAEL values from each reliable study for neurological effects in each species and duration category are recorded in Table 2-1 and plotted in Figure 2-1. Acute exposures HEXACHLOROETHANE 26 2. HEALTH EFFECTS to hexachloroethane appear to cause neurological impairment during exposure of rats and dogs, but symptoms do not persist during the intervals between exposures or after exposure ceases. 2.2.1.5 Reproductive Effects No studies were located regarding reproductive effects in humans after inhalation exposure to hexachloroethane. Hexachloroethane was maternally toxic at concentrations of 48 and 260 ppm in rats exposed 6 hours/day on gestation days 6-16, based on significantly decreased (p value not stated) maternal body weight gain, but it was not embryotoxic or fetotoxic (Weeks et al. 1979). There were no treatment-related gross or histopathological lesions of the testes in rats, dogs, guinea pigs, and quail that were exposed to concentrations of hexachloroethane up to 260 ppm 6 hours/day, 5 days/week for 6 weeks. However, relative testes weights were increased in rats when compared to the controls. No other reproductive organs were evaluated (Weeks et al. 1979). The highest NOAEL from each reliable study for reproductive effects in each species and duration category is recorded in Table 2-1 and plotted in Figure 2-1. 2.2.1.6 Developmental Effects No studies were located regarding developmental effects in humans after inhalation exposure to hexachloroethane. In animals, hexachloroethane did not cause skeletal or soft tissue abnormalities in offspring of rats that were exposed to vapors of hexachloroethane (15-260 ppm) 6 hours/day during gestation days 6-16 (Weeks et al. 1979). The highest NOAEL value from this study for developmental effects in rats is recorded in Table 2-1 and plotted in Figure 2-1. 2.2.1.7 Genotoxic Effects No studies were located regarding genotoxic effects in humans or animals after inhalation exposure to hexachloroethane. Genotoxicity studies are discussed in Section 2.5. HEXACHLOROETHANE 27 2. HEALTH EFFECTS 2.2.1.8 Cancer One case study was identified where a man who had been occupationally exposed to hexachloroethane was treated for a liver tumor (Selden et al. 1989). Exposure had occurred over a period of 6 years as a result of the presence of hexachloroethane in a degassing agent used during aluminum smelting. However, the hexachloroethane reacted at the 700°C use-temperature, releasing a gas that was 96% hexachlorobenzene with small amounts of other chlorinated compounds. Because there was occupational exposure to a mixture of chlorinated compounds rather than just hexachloroethane, it is highly unlikely that the tumor was the result of hexachloroethane exposure alone. Occupational exposure to mineral oil mists for 20 years was also part of the subject's employment history. No studies were located regarding cancer incidence in animals after inhalation exposure to hexachloroethane. EPA has derived an inhalation unit risk (cancer slope factor) of 1.4x102 (mg/kg/day)! for hexachloroethane (IRIS 1995). This inhalation unit risk was calculated using data from oral studies (see Section 2.2.2.8) and Figure 2-2. 2.2.2 Oral Exposure 2.2.2.1 Death No studies were located regarding death in humans after oral exposure to hexachloroethane. When hexachloroethane was administered to rats by gavage with corn oil as the solvent, the LD, value was 5,160 mg/kg for males and 4,460 mg/kg for females (Weeks et al. 1979). Kinkead and Wolfe (1992) reported an LD, value of 4,489 mg/kg for both male and female rats treated with hexachloroethane in corn oil. When hexachloroethane was dissolved in aqueous methyl cellulose solution, the LD, was 7,690 mg/kg for male and 7,080 mg/kg for female rats (Weeks et al. 1979). The lower LD, for the corn oil solvent indicates that the absorption from this hydrophobic medium is greater than that from a hydrophilic medium such as methyl cellulose solution. The LDj, of 4,970 mg/kg for male guinea pigs given hexachloroethane in corn oil is similar to that for rats (Weeks et al. 1979). According to the classification system of Hodge and Sterner (1949), these LDj, values indicate that hexachloroethane is slightly toxic by acute oral exposure. HEXACHLOROETHANE 28 2. HEALTH EFFECTS With repeated administration of hexachloroethane, a dose of 750 mg/kg/day in corn oil was lethal to 1 of 5 male rats and 2 of 5 females within 15 days (NTP 1989). The earliest death occurred in a male rat on day 5. All animals died between day 2 and day 8 with doses of 1,500 and 3,000 mg/kg/day. With 6-week hexachloroethane exposures, there were some deaths among rats given a dose of 1,000 mg/kg/day in corn oil, and all animals died with a dose of 1,780 mg/kg/day (NTP 1977). The number of animals that died at the 1,000 mg/kg/day dose level was not specified and the time of death was not given for any of the doses. There were no deaths in animals given doses of 562 mg/kg/day or lower. Mice were more resistant to hexachloroethane exposure than rats because all of the mice survived doses of 1,000 mg/kg/day in corn oil for 6 weeks (NTP 1977). Some male mice died with a 1,780 mg/kg/day dose, but the exact number was not specified. With a 13-week exposure duration, doses of 750 mg/kg/day in corn oil were lethal to some male and female rats (NTP 1989). The earliest death occurred among the males at 7 weeks. Between 7 weeks and 13 weeks (the end of the exposure period), 5 of 10 males died; during week 13, 2 of 10 females died. Chronic (2-year) exposure of male rats to 20 mg/kg/day hexachloroethane and female rats to 160 mg/kg/day had no effect on survival (NTP 1989), but the longevity of rats exposed to doses of 212 and 423 mg/kg/day for 66 weeks was decreased as compared to controls (NTP 1977; Weisburger 1977). The hexachloroethane was given by gavage in corn oil for both studies. Doses of 750 mg/kg/day and greater can be lethal with both acute- and intermediate-duration exposures, and a chronic intake of 212 mg/kg/day or greater can shorten the lifespan of rats. There were no apparent effects on lifespan with chronic administration of a 160 mg/kg/day dose in female rats or a dose of 20 mg/kg/day in male rats. All identified LOAEL values for lethality in each species and duration category are recorded in Table 2-2 and plotted in Figure 2-2. 2.2.2.2 Systemic Effects The highest NOAEL values and all LOAEL values from each reliable study for systemic effects in each species and duration category are recorded in Table 2-2 and plotted in Figure 2-2. TABLE 2-2. Levels of Significant Exposure to Hexachloroethane - Oral . Exposure LOAEL (effect) Key duration/ to Species frequency NOAEL Less Serious Serious figure (strain) (specific route) System (mg/kg/day) (mg/kg/day) (mg/kg/day) Reference ACUTE EXPOSURE Death 1 Rat Once 4489 (LD50) Kinkead and (Sprague- (GO) Wolfe 1992 Dawley) 2 Rat Once® 7080 F (LD50) Weeks et al. 1979 (Sprague- (G) Dawley) 3 Rat Once’ 7690 M (LD50) Weeks et al. 1979 (Sprague- (G) Dawley) 4 Rat Once 5160 M (LD50) Weeks et al. 1979 (Sprague- (GO) Dawley) 5 Rat Once 4460 F (LD50) Weeks et al. 1979 (Sprague- (GO) Dawley) 6 Gn pig Once (Hartley) (GO) 4970 M (LD50) Weeks et al. 1979 S103443 HLTV3H ¢C 3NVHLIOHOTHOVX3H 62 TABLE 2-2. Levels of Significant Exposure to Hexachloroethane - Oral (continued) ; Exposure LOAEL (effect) Key duration/ to Species frequency NOAEL Less Serious Serious figure (strain) (specific route) System (mg/kg/day) (mg/kg/day) (mg/kg/day) Reference Systemic 7 Rat 11d Resp 100 F S00F (increased mucus in Weeks et al. 1979 (Sprague- Gd 6-16 nasal turbinates; Dawley) (GO) subclinical pneumonitis) Cardio 500 F Gastro 500 F Musc/skel 500 F Hepatic 500 F Derm 500 F Ocular 500 F Bd Wt 100 F 500F (reduced body weight gain, quantitative data not provided) 8 Rabbit 12d Resp 1000 M Weeks et al. 1979 (New (GW) Zealand) Cardio 1000 M Gastro 1000 M Musc/skel 1000 M Hepatic 100¢ M 320M (hepatocellular 1000 M (coagulation; necrosis; degeneration) hemorrhage) Renal 100 M 320M (tubular nephrosis; tubular nephrocalcinosis) Endocr 1000 M Ocular 1000 M Bd Wt 100 M 320M (reduced body weight, quantitative data not provided) S103443 H1V3H “2 3NVHLIOHOTHOVX3H oe TABLE 2-2. Levels of Significant Exposure to Hexachloroethane - Oral (continued) } Exposure LOAEL (effect) Key duration/ to Species frequency NOAEL Less Serious Serious figure (strain) (specific route) System (mg/kg/day) (mg/kg/day) (mg/kg/day) Reference 9 Sheep Once Hepatic 500M (elevated sorbital and Fowler 1969b (GO) glutamate dehydrogenases; ornithine carbamoyl transferase; decreased bromosulphthalein excretion) Neurological 10 Rat Gd 7-17 56 167 F (decreased motor activity) Shimizu et al. (Wistar) (GO) 1992 11 Rat 11d 100 500 F (tremors) Weeks et al. 1979 (Sprague- ~~ Gd 6-16 Dawley) (GO) Reproductive 12 Rat Gd 7-17 167 500 (increased late-stage fetal ~~ Shimizu etal. (Wistar) (GO) resorptions) 1992 13 Rat 11d 100 500 F (increased fetal resorptions; Weeks etal. 1979 (Sprague- Gd 6-16 reduced gestation indices, Dawley) (GO) quantitative data not provided) Developmental 14 Rat Gd 7-17 167 500 (20-25% decrease in fetal ~~ Shimizu etal. (Wistar) (GO) body weights; increase in 1992 skeletal anomalies) 15 Rat 11d 100 500 (delayed development, Weeks et al. 1979 (Sprague- Gd 6-16 details not provided) Dawley) (GO) S103443 H1TV3H ¢ INVHLIOHOTHOVXIH LE TABLE 2-2. Levels of Significant Exposure to Hexachloroethane - Oral (continued) . Exposure LOAEL (effect) Key duration/ to Species frequency NOAEL Less Serious Serious figure (strain) (specific route) System (mg/kg/day) (mg/kg/day) (mg/kg/day) Reference INTERMEDIATE EXPOSURE Death 16 Rat 13 wk 750 B (death of 5/10 males and NTP 1989 (Fischer-344) 5d/wk 2/10 females) (GO) 17 Rat 2-16 d 750 B (death of 1/5 males and 2/5 NTP 1989 (Fischer-344) 5d/wk females) (GO) 1500 B (100% mortality) Systemic 18 Rat 16 wk Resp 62 B Gorzinski et al. (Fischer 344) (F) 1985 Cardio 62 B Gastro 62 B Hemato 62 B Musc/skel 62 B Hepatic 14 B 15M (swelling of hepatocytes in 6/10 males) Renal 1 B 15M (increased kidney weight 10%; increased relative kidney weight 5.5%; tubular atrophy and hypertrophy) Endocr 62 B Derm 62 B Ocular 62 B Bd Wt 62 B 19 Rat 7 wk Hepatic 497M (significantly increased Milman et al. (Osbome- ~~ 5d/wk mean liver weight) 1988; Story et al. Mendel) (GO) 1986 INVHLIOHOTHOVYX3H S103443 H1V3aH 2 [4 TABLE 2-2. Levels of Significant Exposure to Hexachloroethane - Oral (continued) } Exposure LOAEL (effect) Key duration/ to Species frequency NOAEL Less Serious Serious figure (strain) (specific route) System (mg/kg/day) (mg/kg/day) (mg/kg/day) Reference 20 Rat 6 wk Bd Wt 316 562M (decreased body weight 1000 M (38% decreased body NTP 1977 (Osbome- ~~ Sd/wk gain, amount not weight gain) Mendel) (GO) specified) 21 Rat 2-16 d Resp 375 B 750 B (shortness of breath) NTP 1989 (Fischer-344) 5d/wk (GO) Renal 187M (hyaline droplet formation; granular cast) Ocular 375 B 750B (lacrimation) Bd Wt 375 B 750 B (mean body weight decreased 24% in females; males gained 24% of the amount gained by controls) 22 Rat 13 wk Resp 750 B NTP 1989 (Fischer-344) 5d/wk (GO) Cardio 750 B Gastro 750 B Hepatic 9 B 188 F (centrilobular necrosis and increased liver weight) Renal 47M (hyaline droplets; tubular degeneration) Derm 750 B Ocular 750 B Bd Wt 375 B 750M (19% reduction in mean body weight) 23 Mouse 6 wk Bd Wt 1000 B 1780B (reduced body weight NTP 1977 (B6C3F1) 5d/wk gain, quantitative data (GO) not provided) S103443 HLTV3H ¢ ANVHL3OHOTHOVX3H €e TABLE 2-2. Levels of Significant Exposure to Hexachloroethane - Oral (continued) ; Exposure LOAEL (effect) Key duration/ to Species frequency NOAEL Less Serious Serious figure (strain) (specific route) System (mg/kg/day) (mg/kg/day) (mg/kg/day) Reference Neurological 24 Rat 13 wk 47 B 94B (post-gavage 375 B (convulsions) NTP 1989 (Fischer-344) 5d/wk hyperactivity) (GO) CHRONIC EXPOSURE Death 25 Rat 66 wk 212 B (26/50 males and 23/50 NTP 1977; (Osborne- 5d/wk females died before the end Weisburger 1977 Mendel) (GO) of the study) Systemic 26 Rat 66 wk Renal 212 B (tubular necrosis; interstitial NTP 1977; (Osborne- 5d/wk nephritis; regenerative Weisburger 1977 Mendel) (GO) epithelium; fibrosis and casts) Bd Wt 212 M (30% reduction of weight gain) 27 Rat 2yr Resp 160 F NTP 1989 (Fischer-344) 5d/wk (GO) Cardio 160 F Gastro 160 F Hepatic 160 F Renal 10M (mineralization of renal 20 M (necrosis; regenerative papillae; renal tubule epithelium; interstitial hyperplasia) fibrosis) Derm 160 F S103443 H1TV3H “2 INVYHLIOHOTHOVX3H ye TABLE 2-2. Levels of Significant Exposure to Hexachloroethane - Oral (continued) ; Exposure LOAEL (effect) Key duration/ to Species frequency NOAEL Less Serious Serious figure (strain) (specific route) System (mg/kg/day) (mg/kg/day) (mg/kg/day) Reference 28 Mouse 78 wk Renal 590 B (tubular nephropathy; NTP 1977; (B6C3F1) 5d/wk degeneration of the tubular ~~ Weisburger 1977 (GO) epithelium; inflammation, fibrosis; calcium deposits) Bd Wt 590 B Cancer 29 Rat 2yr 20 M (CEL: renal tubular NTP 1989 (Fischer-344) 5d/wk adenoma or (GO) adenocarcinoma in 7/50) 10 M (CEL: pheochromocytomas in adrenal gland 28/45) 30 Mouse 78 wk 590 B (CEL: hepatocellular NTP 1977; (BBC3F1) 5d/wk carcinomas 35/50) Weisburger 1977 (GO) "The numbers correspond to entries in Figure 2-2. ®Administered in methylcellulose solution. Used to derive an acute-duration oral minimal risk level (MRL) of 1 mg/kg/day; dose divided by an uncertainty factor of 100 (10 for extrapolation from animals to humans and 10 for human variability). Used to derive an intermediate-duration oral MRL of 0.01 mg/kg/day; dose divided by an uncertainty factor of 100 (10 for extrapolation from animals to humans and 10 for human variability). B = both; Bd Wt = body weight; Cardio = cardiovascular; CEL = cancer effect level; d = day(s); Derm = dermal; Endocr = endocrine; F = female; (F) = food; (G) = gavage; Gastro = gastrointestinal; Gd = gestation day(s); Gn pig = guinea pig; (GO) = gavage oil; (GW) = gavage water; Hemato = hematological; LD50 = lethal dose (50% kill); LOAEL = lowest-observed-adverse-effect level; M = male;; Musc/skel = musculoskeletal; NOAEL = no-observed-adverse-effect level; Resp = respiratory; wk = week(s); yr = year(s) S103443 H1TV3H ¢ ANVHLIOHOTHOVX3IH SE Figure 2-2. Levels of Significant Exposure to Hexachlorethane - Oral Acute (<14 days) Systemic $2 0 Wo ae x > 2 N ® > © 2 x) cr & F&F FF oo & A e eS F&F (mg/kg/day) RS FF OF Fd FE OF f° & & LFF Sf LL & SS» > RK ot Q *T TU WF FE QC Q < ® Jd 10,000 — = 1r 4r 5.69 1.000 — S889 2 a 9 8h TOT OT OM 0 Mo oO O d ee 0 00 r 7 nr r 7c 9a P wT Tr 0 ° 1r rs 13r oe 8h — oO O Osh O O 100 Q@ QO &@ 7r 8h 107 47; 12r a1 191 15 8h | O 1 10r 6 [~ | | 1 [~ Vv 0.1 Key r Rat BM LDs0 The number next to m Mouse i ; each point corresponds 0.01 ny @ LOAEL for serious effects (animals) 16 entries ini Table 2-2. . g Guinea pig (D LOAEL for less serious effects (animals) h Rabbit O NOAEL (animals) ! Minimal risk level for effects 0.001 — a Sheep % CEL - Cancer Effect Level (animals) J ste tian cancer “Doses represent the lowest dose tested per study that produced a tumorigenic response and do not imply the existence of a threshold for the cancer end point. S103443 H1TV3H 2 INVHLIOHOTHOVX3H 9€ Figure 2-2. Levels of Significant Exposure to Hexaxhlorethane - Oral (continued) Intermediate (15-364 days) Systemic > > N CI Q SN 0 i’ 2 3 & OO FY OOF § > S : wo QO N O (mg/kg/day) QS & &S © & > > oF NE & © ® FP > >° & ¥ XN & SO 2 F SO > FF ff FF C9 0 Q 10,000 ee 17r or 23m 1.000 I= 21r 20 og 27 2 a ' e® O00 O O oO dO pT ® Pom 24r werize O 22r 22 22 @ 22 2r QQ 2 o 0 O ° 1r vr @ OO 21r oy OF = 100 [— 0 21r r > oO O O OO 251 pO O O O O24 18r 18r 18r 18r 18r 22r 18r 18r 18r 18r o4r 10 | > @ 18r 18r 1.0 f= O 0 18r Q | 0.1} | I | 0.0% ™ oc Key 0.001 }— r Rat B LDs0 The number next to m Mouse ; : each point corresponds hy @ LOAEL for serious effects (animals) to entries in Table 2-2. 0.0001 L— g Quinea pig (DP LOAEL for less serious effects (animals) ‘ h Rabbit O NOAEL (animals) ! Minimal risk level for effects a Sheep & CEL - Cancer Effect Level (animals) 3 oibeiiinen cancer *Doses represent the lowest dose tested per study that produced a tumorigenic response and do not imply the existence of a threshold for the cancer end point. INVHL3IOHOTHOVX3H S103443 H1TV3H 2 LE Figure 2-2. Levels of Significant Exposure to Hexachlorethane - Oral (continued) (mg/kg/day) 1,000 100 10 1 0.1 0.01 0.001 0.0001 0.00001 0.000001 Chronic (>365 days) Systemic $f Q Q SN a SN O 9 Q 9 h S$ Q .O N RN < > CO OAS >» & 2 F © 8 > SEE) ¢ 2 PR & Q & & O° 7 © Se 32 M (LD50) g/kg 132 M mg/kg 100 mg M (corneal opacity; iritis) 1000 M (no skin sensitization) ppm Weeks et al. 1979 Weeks et al. 1979 Weeks et al. 1979 Weeks et al. 1979 S103443 H1IV3aH ¢ INVHLIOHOTHOVX3H Derm = dermal; Gn pig = guinea pig;; hr = hour(s); LD50 = lethal dose (50% kill); LOAEL = lowest-observed-adverse-effect level; M = male; NOAEL = no-observed-adverse-effect level; wk = week(s) 1S HEXACHLOROETHANE 52 2. HEALTH EFFECTS Hepatic Effects. Liver function tests (serum bilirubin, alkaline phosphatase, aspartate aminotransferase, alanine aminotransferase, gamma-glutamyl transferase) completed in 11 hexachloroethane workers who wore protective clothing were within the normal range (Selden et al. 1994). Mild skin and mucous membrane irritation were reported in the exposed group, suggesting that exposure may have been through either the inhalation or dermal routes of exposure. No studies were located regarding hepatic effects in animals after dermal exposure to hexachloroethane. Renal Effects. Renal function tests (serum creatinine and urate, urinary hemoglobin, protein and glucose) completed in 11 hexachloroethane workers who wore protective clothing were within the normal range (Selden et al. 1994). Mild skin and mucous membrane irritation were reported in the exposed group, suggesting that exposure may have been through either the inhalation or dermal routes of exposure. No studies were located regarding renal effects in animals after dermal exposure to hexachloroethane. Dermal Effects. Hexachloroethane-exposed workers reported a slightly higher prevalence of dry skin and dry mucous membranes as well as itching and other skin problems than the unexposed controls (Selden et al. 1994). Clinical examinations of the 11 exposed workers did not reveal signs of abnormal dermatological status. Plasma hexachloroethane levels in these workers, who wore protective equipment, were 7.3 + 6.04 ug/L at the time of the examinations (Selden et al. 1993). The investigators indicate that the dermal effects may also have been a result of a local trauma effect of the protective equipment. Hexachloroethane had no effects on intact or abraded skin of rabbits when 500 mg was applied to shaved skin as the pure solid (Weeks et al. 1979). There was only a slight redness at the application site when it was applied as a water paste. All redness disappeared after 72 hours. The NOAEL for dermal effects in rabbits (132 mg/kg) is reported in Table 2-3. Ocular Effects. No studies were located regarding ocular effects in humans after dermal exposure to hexachloroethane. HEXACHLOROETHANE 53 2. HEALTH EFFECTS Contact with crystalline hexachloroethane (100 mg caused swelling, iritis, corneal opacity, and discharge when placed in rabbit eyes overnight. All signs of ocular irritation were reversed 72 hours later (Weeks etal. 1979). This LOAEL for ocular effects in rabbits is reported in Table 2-3. Contact with hexachloroethane vapors at a concentration of 260 ppm was apparently irritating to the eyes of dogs because the animals kept their eyes closed during all exposure periods (Weeks et al. 1979). In rats, a red exudate was observed about the eyes after 4 weeks of exposure to hexachloroethane vapors, and in rabbits, after a single dermal exposure to a water paste of hexachloroethane (Weeks et al. 1979). The red exudate did not appear until after 4 weeks of exposure to hexachloroethane vapor and, thus, may be a systemic effect rather than the effect of direct contact of the eye with hexachloroethane. 2.2.3.3 Immunological and Lymphoreticular Effects No studies were located regarding immunological or lymphoreticular effects in humans following dermal exposure to hexachloroethane. Hexachloroethane did not act as a sensitizer in guinea pigs when a challenge dose was given 2 weeks after the end of a 3-week sensitization period (Weeks et al. 1979). Accordingly, it did not stimulate antibody formation during sensitization. The NOAEL for dermal sensitization is reported in Table 2-3. 2.2.3.4 Neurological Effects No studies were located regarding neurological effects in humans following dermal exposure to hexachloroethane. Rats that died after dermal exposure to unspecified doses of hexachloroethane during an LD test protocol displayed ataxia, tremors, and convulsions before death (Weeks et al. 1979). HEXACHLOROETHANE 54 2. HEALTH EFFECTS No studies were located regarding the following health effects in humans or animals after dermal exposure to hexachloroethane: 2.2.3.5 Reproductive Effects 2.2.3.6 Developmental Effects 2.2.3.7 Genotoxic Effects Genotoxicity studies are discussed in Section 2.5. 2.2.3.8 Cancer No studies were located regarding cancer in humans or animals after dermal exposure to hexachloroethane. 2.3 TOXICOKINETICS Hexachloroethane has been found in the plasma of workers wearing protective clothing and respiratory protection suggesting that hexachloroethane can be absorbed following inhalation and/or dermal exposure. Based on the minimal effects seen on target tissues (liver and kidney) in animal studies, absorption from the lungs seems to be limited. Dermal absorption was also estimated to be low based on calculated dermal penetration rates. Data on absorption across the gastrointestinal tract indicate that hexachloroethane is absorbed, but the percentage of a dose that is absorbed varies. Absorption estimates based on excretory products in rabbits suggest that a moderate portion of a 500 mg/kg dose (perhaps 40-50%) is absorbed. Data on excretory products from rats and mice indicate that a much larger portion (62-88%) of this same dose is absorbed. Hexachloroethane distributes preferentially to the adipose tissue. Relatively high concentrations are also found in male rat kidneys. Moderate concentrations of hexachloroethane are found in the liver, female kidney, and blood and small amounts in muscle, lungs, and brain. If the hexachloroethane is generated endogenously from carbon tetrachloride, the concentration in the rat liver exceeds that in the kidneys. HEXACHLOROETHANE 55 2. HEALTH EFFECTS Hexachloroethane is metabolized by the mixed function oxidase system by way of a two-step reduction reaction involving cytochrome P-450 and either reduced nicotinamide adenine dinucleotide phosphate (NADPH) or cytochrome bs as an electron donor. The first step of the reduction reaction results in the formation of the pentachloroethyl free radical. In the second step, tetrachloroethene is formed as the primary metabolite. Two chloride ions are released. Pentachloroethane is a minor metabolic product that is generated from the pentachloroethyl free radical. The primary metabolites of hexachloroethane are eventually oxidized to form trichloroethanol and trichloroacetic acid. These ultimate metabolites are excreted along with unchanged hexachloroethane, tetrachloroethene, and pentachloroethane. A small amount of the absorbed hexachloroethane is oxidized completely to carbon dioxide. Hexachloroethane and its metabolites are removed from the body in exhaled air, urine, and bile. In rats and mice, 60-70% of the radiolabeled hexachloroethane was in exhaled air and was present as volatiles other than carbon dioxide. 2.3.1 Absorption 2.3.1.1 Inhalation Exposure No information was located regarding absorption in either humans or animals after inhalation exposure to hexachloroethane. The minor effects of hexachloroethane on organs other than the lungs in animal studies indicates that absorption does occur, but is probably minimal. Given the lipophilic nature of hexachloroethane, absorption across the lung epithelium is possible. 2.3.1.2 Oral Exposure No studies were located regarding absorption in humans following oral exposure to hexachloroethane. When sheep were administered a dose of 500 mg/kg hexachloroethane dissolved in olive oil and emulsified in water, absorption was slow based on the appearance of hexachloroethane in the venous blood (Fowler 1969b). The maximum concentration in blood was observed 24 hours after compound administration in one sheep. HEXACHLOROETHANE 56 2. HEALTH EFFECTS Based on the amount of label found in rabbit urine and exhaled air, 19-29% of a 500 mg/kg dose was absorbed (Jondorf et al. 1957). Since some hexachloroethane would be excreted in bile and found in fecal matter, the actual amount absorbed was larger than 30%, perhaps 40-50%. Data from studies in rats and mice using '*C-radiolabeled hexachloroethane suggest that much higher proportions of a 500 mg/kg/day dose of hexachloroethane were absorbed (Mitoma et al. 1985). Rats exhaled 65% of the radiolabel in expired air and 6% in the excreta. This indicates that more than 65-70% of the hexachloroethane was absorbed. Comparable data from mice given 999 mg/kg/day indicate that more than 72-88% of the dose was absorbed. The radiolabel in expired air was 72% of the dose in mice and there was 16% of the label in the excreta (Mitoma et al. 1985). Hexachloroethane is apparently absorbed to a greater extent when administered in corn oil than when administered in an aqueous medium, based on the fact that the LD, values for hexachloroethane dissolved in methyl cellulose solution are higher than those for a corn oil solvent in both male and female rats (Weeks et al. 1979). The ratio of LD, values suggests that about one-third less material is absorbed from an aqueous medium. 2.3.1.3 Dermal Exposure Despite wearing protective equipment that included disposable overalls and compressed-air-fed visors or full-facepiece masks with filters for dusts and vapors, hexachloroethane was detected in the plasma of exposed workers (Selden et al. 1993). After 5 weeks of exposure, plasma levels of hexachloroethane in 12 workers were 7.3 + 6 pg/L. Mild dermal irritation was also noted. If the skin irritation was a response to hexachloroethane rather than trauma from the protective clothing, the irritation suggests that the principal exposure route may have been dermal. Absorption of a saturated hexachloroethane solution across human skin was estimated to be 0.0230 mg/cm? hour based on the physical properties of hexachloroethane (Fiserova-Bergerova et al. 1990). No information was located regarding absorption of hexachloroethane in animals after dermal exposure. HEXACHLOROETHANE 57 2. HEALTH EFFECTS 2.3.2 Distribution 2.3.2.1 Inhalation Exposure No information was located regarding distribution in humans or animals following inhalation exposure to hexachloroethane. 2.3.2.2 Oral Exposure No information was located regarding distribution in humans following oral exposure to hexachloroethane. After oral exposure of rats to hexachloroethane for 8-16 weeks, the largest concentration of hexachloroethane was found in the adipose tissues (Gorzinski et al. 1985; Nolan and Karbowski 1978). The kidneys of male rats, but not females, also contained high concentrations of hexachloroethane. When rats were given doses of 3, 30, or 100 mg/kg/day for 110-111 days, the concentration in the male kidney was four times larger than that in the female kidney at the lowest dose and 48 times larger at the highest dose (Nolan and Karbowski 1978). These proportions are very much like the relationship found with doses of 1, 15, or 62 mg/kg/day given to rats where the male kidney contained four times as much label as the female kidney at the low dose and 45 times as much as the female kidney at the high dose (Gorzinski et al. 1985). Hexachloroethane is also found in the liver and blood after oral exposure to hexachloroethane, although the levels found in these tissues are much lower than those found in adipose tissue and male rat kidney (Gorzinski et al. 1985; Nolan and Karbowski 1978). With a dose of 1 mg/kg/day, adipose tissue samples from male rats contained 3.15 pg/g; the kidneys contained 1.36 ug/g; the liver, 0.29 pg/g; and the blood, 0.08 ng/g after 16 weeks of exposure (Gorzinski et al. 1985). In the female rat, the adipose tissue contained 2.59 ug/g; the kidneys, 0.39 pg/g; the liver, 0.26 ug/g; and the blood, 0.07 pg/g. As the doses were increased, the concentrations in the tissues also increased. There is a relatively rapid turnover of hexachloroethane in the tissues. In studies where doses of 62 or 100 mg/kg/day hexachloroethane were fed in the diet for about 8 weeks, the level in the tissue decayed HEXACHLOROETHANE 58 2. HEALTH EFFECTS with a half-life of 2.3-2.7 days following first order kinetics (Gorzinski et al. 1985; Nolan and Karbowski 1978). In sheep fed hexachloroethane in olive oil emulsified in water, the hexachloroethane was found primarily in the liver, kidneys, and adipose tissue 8 hours after exposure; much smaller amounts were found in brain and muscle 8 hours after exposure. The maximum concentration of hexachloroethane in blood occurred 24 hours after dosing (Fowler 1969b). 2.3.2.3 Dermal Exposure No information was located regarding distribution in humans or animals after dermal exposure to hexachloroethane. 2.3.2.4 Other Routes of Exposure The tissue distribution of intraperitoneal '“C hexachloroethane in male rats differed from that in male mice based on the concentrations that were bound to DNA, RNA, and protein (Lattanzi et al. 1988). In both species the highest concentrations of label were found in the kidney, followed by the liver, lungs, and stomach in descending order. The amount of bound label in the mice, however, was about twice that in the rat for both kidney and liver. The higher concentration of label in mouse liver may help to explain why hepatocellular cancer has been seen in mice but not in rats. Hexachloroethane can be generated endogenously from exposure to carbon tetrachloride. Hexachloro- ethane is formed in the liver through the union of two trichloromethyl free radicals. The tissue distribution of endogenously generated hexachloroethane differed from that of exogenous hexachloroethane. After oral administration of 1 mL/kg carbon tetrachloride to rabbits, adipose tissue contained the highest concentration of hexachloroethane (4.1 + 1.2, 16.5 + 1.6, and 6.8 + 2.4 ng/g) at 6, 24, and 48 hours (Fowler 1969a). This was similar to the distribution found after oral and intraperitoneal exposure to hexachloroethane (Gorzinski et al. 1985; Lattanzi et al. 1988; Nolan and Karbowski 1978). However, the amount in the liver was about twice that in the kidney at both 6 and 24 hours. At 6 hours, the liver contained 1.6 + 0.5 ng/g and the kidney 0.7 + 0.2 ng/g, while at 24 hours the liver contained 4.2 + 1.8 ng/g and the kidney contained 2.2 + 1.1 ng/g (Fowler 1969a). Only small amounts were found in the muscle. HEXACHLOROETHANE 59 2. HEALTH EFFECTS 23.3 Metabolism Most of the information on the metabolism of hexachloroethane has been collected by in vitro techniques using rat liver slices or rat liver microsomes. Figure 2-3 summarizes the results of these studies. The identification of tetrachloroethene and pentachloroethane as the initial metabolites of hexachloroethane metabolism in vitro agrees with in vivo data from sheep that were orally exposed to doses of 500—1,000 mg/kg hexachloroethane (Fowler 1969b). The initial steps of hexachloroethane metabolism take place in liver microsomes under anaerobic conditions (Nastainczyk et al. 1982a, 1982b; Salmon et al. 1981, 1985; Town and Leibman 1984). Cytosolic enzymes are minimally involved with hexachloroethane metabolism (Town and Leibman 1984). Hexachloroethane is dechlorinated in a two-step reduction reaction. In the first step, cytochrome P-450 contributes one electron to hexachloroethane, leading to the loss of a chloride ion and the formation of a pentachloroethyl free radical. In the second step, a second electron is contributed by either NADPH or cytochrome bs and a second chloride is lost, producing tetrachloroethene (Nastainczyk et al. 1982a). A smaller amount of the pentachloroethyl free radical becomes pentachloroethane by abstraction of a hydrogen atom from a hydrogen donor. In studies using liver microsomes, approximately 99.5% of the hexachloroethane was converted to tetrachloroethene at physiological pHs (Nastainczyk et al. 1982b). When the reaction occurred at higher pHs (8.4-8.8), the ratio of pentachloroethane to tetrachloroethene was increased. The specific cytochrome P-450 involved in this series of reactions was stimulated by phenobarbital and not by 3-methylchloanthrene (Nastainczyk et al. 1982a; Salmon et al. 1985; Thompson et al. 1984; Town and Leibman 1984). Both tetrachloroethene and pentachloroethane undergo subsequent hepatic metabolism. Pentachloroethane is reductively dechlorinated by microsomes to yield trichloroethene. (Reductive dechlorination was favored when there were three chlorines on one carbon and at least one chlorine on the vicinal carbon [Thompson et al. 1984], a characteristic shared by hexachloroethane and pentachloroethane). Trichloroethene and tetrachloroethene were then oxidized by hepatic enzymes to form trichloroethanol and trichloroacetic acid as terminal reaction products. Apparently additional dechlorination reactions can occur since labeled dichloroethanol, dichloroacetic acid, monochloroacetic acid, and oxalic acid have been HEXACHLOROETHANE 60 2. HEALTH EFFECTS FIGURE 2-3. Metabolism of Hexachloroethane Cl Cl Cl - c x ¢ - Cl Cl CI Hexachloroethane Cytochrome P-450 Cr at Sl Cl = G5 Cl Cl Pentachloroethyl Free Radical NADPH cr Ar a cl ol Cl-C-C-H Cl Cl I =C Cl Cl - N Cl Cl Pentachloroethane Tetrachloroethene ’ Cl Cl > C= C_ Cl H Trichloroethene Cl Oo Cl H | 7 | | 8l-C-C Cl-G-G-OH | Cl OH Cl H Trichloroacetic Acid Trichloroethanol HEXACHLOROETHANE 61 2. HEALTH EFFECTS found in the urine of animals given an oral dose of labeled hexachloroethane (Jondorf et al. 1957; Mitoma et al. 1985). Some hexachloroethane (about 2%) was completely dechlorinated and metabolized to carbon dioxide in rats and mice (Mitoma et al. 1985). 23.4 Excretion 2.3.4.1 Inhalation Exposure No data were located regarding excretion in humans or animals after inhalation exposure to hexachloroethane. 2.3.4.2 Oral Exposure Orally ingested hexachloroethane is exhaled and excreted in urine and fecal matter. The portion of the hexachloroethane found in fecal matter is the result of excretion in bile. The results of studies that measured the amount of residual hexachloroethane in excreta can be misleading, since much of the absorbed hexachloroethane is metabolized to other compounds. Measurement of 1C label after exposure to labeled compound presents a more complete picture of ultimate hexachloroethane fate and excretion than measurement of hexachloroethane. In rats and mice, 65-70% of an oral dose of radiolabeled hexachloroethane (500 mg/kg/day for rats and 999 mg/kg/day for mice) was present in exhaled air (Mitoma et al. 1985). Only about 2% of this amount was exhaled as carbon dioxide. The remainder was present as other volatile compounds. In rabbits, a much smaller portion of the label was found in exhaled air (14-24%) after oral administration of 500 mg/kg hexachloroethane. The amount of labeled carbon dioxide was not determined (Jondorf et al. 1957). Relatively little hexachloroethane, pentachloroethane, and tetrachloroethene was found in the urine of sheep after oral administration of 500 mg/kg hexachloroethane (Fowler 1969b), and relatively little label (5%) was found in the urine of rabbits given 500 mg/kg (Jondorf et al. 1957). The major urinary metabolites were trichloroethanol and trichloroacetic acid in rats, rabbits, and mice (Jondorf et al. 1957, Mitoma et al. 1985). In rabbits, smaller amounts of dichloroethanol, dichloroacetic acid, monochloroacetic acid, and oxalic acid were also present (Jondorf et al. 1957). HEXACHLOROETHANE 62 2. HEALTH EFFECTS In sheep, 80% of the hexachloroethane, tetrachloroethene, and pentachloroethane fecal excretions were excreted within 24 hours (Fowler 1969b). Some of this was unabsorbed hexachloroethane and the remainder was material that had been absorbed and was excreted with the bile. Hexachloroethane was present in bile within 15 minutes of dosing and the concentration in bile was 8=10 times greater than that in blood at that time. Traces of hexachloroethane, tetrachloroethene, and pentachloroethane were present in the 48-72 hour fecal collections. 2.3.4.3 Dermal Exposure No studies were located regarding excretion by humans or animals after dermal exposure to hexachloroethane. 2.4 Mechanisms of Action The kidney and liver are the primary target organs for hexachloroethane based on the results of toxicity testing and supported by toxicokinetic information from tissue distribution and binding studies (Lattanzi et al. 1988). Male rats were more susceptible to kidney damage than female rats (NTP 1989), and the kidneys of male rats contained 4-45% more hexachloroethane radiolabel than the kidneys of female rats (Gorzinski et al. 1985). However, there were some effects on kidneys of both sexes. * The mechanism of toxicity leading to tubular nephropathy and renal tumorigenesis in male rats is related to the synthesis and excretion of the protein a2u-globulin. This protein is synthesized in the liver and secreted into the blood. It is filtered through the glomeruli of the kidneys and partially reabsorbed through the proximal tubules where it is partially hydrolyzed (Swenberg 1993). The remainder is excreted, comprising 26% of the urinary protein (NTP 1989; Olson et al. 1990). Other species of laboratory animals, female rats, and humans produce minimal amounts of an a2u-globulin-type protein. In the presence of hexachloroethane and other nonpolar hydrocarbons or their metabolites, a2p-globulin accumulates in hyaline droplets in the tubular epithelium. The accumulation of hyaline droplets damages the epithelial cells, leading to exfoliation and the appearance of hyaline casts in the urine. Regenerative repair of the epithelium leads to hyperplasia and increases the risk for tumors when mutated cells divide before DNA repair can occur. HEXACHLOROETHANE 63 2. HEALTH EFFECTS Although binding of hexachloroethane to a2u-globulin can explain kidney damage in male rats, it does not explain the less severe kidney changes in female rats (NTP 1989). Thus, other mechanisms must be involved in the nephrotoxicity of hexachloroethane. When DNA, RNA, and protein were isolated from kidney cells of male rats, it was found that hexachloroethane was bound more strongly to RNA and protein than to DNA (Lattanzi et al. 1988). The highest concentrations were found bound to RNA. Epigenetic interference with protein synthesis and cell function could lead to the kidney nephropathy seen in female rats and contribute to the damage in male rats. However, no studies were identified that would support this hypothetical mechanism. Liver necrosis is another concern following hexachloroethane exposure. Hexachloroethane is metabolized in the centrilobular area of the liver by way of the microsomal mixed function oxidase system. The relatively nonpolar pentachloroethyl free radical is an intermediate in this pathway. The reaction of the free radical with unsaturated lipids in the cellular or organelle membranes could contribute to hepatocyte damage and necrosis. Conjugated dienes and malondialdehyde serve as a markers for free radical-induced lipid peroxidation. There was a uniform increase in malondialdehyde in eight assays of rat liver microsomes that were incubated with hexachloroethane (Town and Leibman 1984). Conjugated dienes were increased in some, but not all, of the samples. No changes were seen in the concentration of conjugated dienes in the hepatic endoplasmic reticulum of male rats, 2 hours after hexachloroethane exposure (Reynolds 1972). The authors hypothesized that the poor solubility of hexachloroethane in body fluid and the use of a mineral oil solvent limited the concentration of hexachloroethane in the liver at 2 hours and, thus, the lack of its effects on conjugated dienes could not be used to eliminate the possibility of free radical cellular damage at a later point in time. Although limited, the data provide some support for a free radical mechanism for the hepatic toxicity of hexachloroethane. Clinical signs of neurotoxicity (tremors and ataxia) have been observed in sheep, dogs, and rats during or immediately after both oral and inhalation exposure. Sometimes tremors developed early in the treatment regime and other times the tremors became apparent only after repeated exposures. Fluke-infected sheep experienced tremors of the facial muscles, neck, and forelimbs and were unable to stand after treatment with hexachloroethane. They were successfully treated with calcium borogluconate. This suggests that the neurological action of hexachloroethane may be the result of interference with the availability of calcium within excitable cells. HEXACHLOROETHANE 64 2. HEALTH EFFECTS 2.5 RELEVANCE TO PUBLIC HEALTH Hexachloroethane is a solid crystalline material that has entered the environment as a result of its use in military pyrotechnics and as a component of smoke-producing devices used for screening or signaling purposes. Itis an intermediate in the production of fluorocarbons, cleaning agents, and refrigerants and was once used in veterinary medicine to control liver flukes in sheep. It can be found at military disposal sites and at hazardous waste sites. In addition, hexachloroethane can be formed during incineration of chlorinated organic compounds and during chlorination of drinking water. Accordingly, there is some risk that humans can be exposed to this material. Respiratory, hematological, liver, and renal effects were not observed in 11 hexachloroethane-exposed workers. The identification of hexachloroethane in the plasma of these workers confirmed exposure, although the workers were wearing protective equipment. Mild dermal irritation was noted that may have been from exposure or a result of a local trauma effect of the protective equipment. Animal studies identify the kidney and liver as the primary target organs for hexachloroethane. Renal problems were most severe in male rats and were associated with a2p-globulin/hyaline droplet nephropathy. Minimal to mild lesions were also seen in female rat kidneys and in male and female mice, indicating that some mechanism, in addition to hyaline droplet formation, is involved in renal toxicity. The liver responds to hexachloroethane exposure with increases in liver weight, increases in serum levels of liver enzymes, centrilobular necrosis, fatty degeneration, hemosiderin-laden macrophages, and hemorrhage. Effects on the liver and kidneys were mild with inhalation exposure and more pronounced with oral exposure. No data were available for effects on the liver and kidneys by the dermal exposure route. Hexachloroethane vapors and ingested hexachloroethane act as irritants on the lining of the lung, nasal cavity, trachea, and other tissues of the respiratory tract. Pulmonary irritation was associated with an increased incidence of mycoplasma infection in rats. Hexachloroethane exposure can also irritate the eyes. The irritation of the eye and respiratory tract are reversible once exposure has ceased. Both oral and inhalation exposures to high concentrations of hexachloroethane were associated with hyperactivity, ataxia, convulsions, and/or prostration in rats, sheep, and dogs. The mechanism for these HEXACHLOROETHANE 65 2. HEALTH EFFECTS neurological effects is not clear since there were no apparent histopathological lesions in the brains of the affected animals. Neurological effects were only noted with the high-dose exposures. There has been no comprehensive evaluation of the reproductive and developmental effects of hexachloroethane. Limited data indicate that it is maternally toxic and retards fetal development. It does not appear to be a teratogen. Minimal Risk Levels for Hexachloroethane Inhalation MRLs e An MRL of 6 ppm has been derived for acute inhalation exposure to hexachloroethane. This MRL is based on a study in pregnant female rats exposed to concentrations of 0, 15, 48, or 260 ppm hexachloroethane for 6 hours/day on gestation days 6-16 (Weeks et al. 1979). Tremors were observed in the 260-ppm dose group during exposure starting on day 12 and persisting through day 16. Excess mucus was present in the nasal turbinates of all of the dams in the 260-ppm dose group and 85% of the dams in the 48-ppm dose group. This effect was not observed at 48 ppm in the 6-week study, and the endemic mycoplasma infection that was present in the colony of rats used in the Weeks et al. (1979) study may have contributed to this effect. Based on the NOAEL of 48 ppm for neurological effects observed in the teratology study by Weeks et al. (1979), an acute inhalation MRL was calculated by adjusting to a Human Equivalent Concentration (HEC) of 181 ppm using reference ventilation rates (rat, 0.22 m’/day; human, 20 m*/day) and body weights (rat, 0.204 kg; human, 70 kg) from EPA (1988a) and by dividing by an uncertainty factor of 30. A factor of 3 was used to extrapolate from animals to humans, and a factor of 10 was used to account for human variability. e An MRL of 6 ppm has been derived for intermediate-duration inhalation exposure to hexachloroethane. This MRL is based on the 6-week study in rats by Weeks et al. (1979) in which tremors were observed at 260 ppm but not at 48 ppm. Based on the NOAEL of 48 ppm for neurological effects observed in the 6-week study (Weeks et al. 1979), an intermediate inhalation MRL was calculated by adjusting the NOAEL to an HEC of 174 ppm using reference ventilation rates (rat, 0.245 m*/day; human, 20 m’/day) and body weights (rat, 0.236 kg; human, 70 kg) from EPA (1988a) and by dividing by an uncertainty factor of 30. A factor of 3 was used HEXACHLOROETHANE 66 2. HEALTH EFFECTS to extrapolate from animals to humans, and a factor of 10 was used to account for human variability. A chronic MRL for inhalation exposure has not been derived because no data were located on the effects of long-term exposures in humans or animals. Oral MRLs ® An MRL of 1 mg/kg/day has been derived for acute oral exposure to hexachloroethane. This MRL was derived from a NOAEL of 100 mg/kg/day in a study where groups of five male New Zealand rabbits were given doses of 0, 100, 320, and 1,000 mg/kg/day hexachloroethane dissolved in methyl cellulose solution by gavage for 12 days (Weeks et al. 1979). Dose- dependant liver degeneration and necrosis were noted at dose levels of 320 and 1,000 mg/kg/day. Effects were characterized as fatty degeneration, coagulation necrosis, hemorrhage, ballooning degeneration, eosinophilic change, hemosiderin-laden macrophages and giant cells. Comparable effects were not seen in the 100-mg/kg/day dose group. Liver weights increased at the highest dose tested; however, quantitative data were not provided. The NOAEL of 100 mg/kg/day was divided by an uncertainty factor of 100, 10 each for interspecies and intraspecies variability. Toxic tubular nephrosis and minimal nephrocalcinosis of the convoluted tubules were seen at dose levels of 320 and 1,000 mg/kg/day, however comparable effects were not seen at the lowest dose tested. Kidney weights increased significantly (p<0.05) at the highest dose tested. For the most part, serum clinical parameters (blood urea nitrogen, protein bilirubin, aspartate amino- transferase, alanine aminotransferase, alkaline phosphatase, and sodium) were not affected significantly. Levels of potassium and glucose were decreased significantly at dose levels of 320 mg/kg/day or greater. Body weights were reduced significantly (p<0.05) at exposure levels of 320 and 1,000 mg/kg/day. Quantitative data were not provided for any of the effects noted in this study, although the degree of significance and the dose-related nature of the effects were included in the discussion of the results. ® An MRL of 0.01 mg/kg/day has been derived for intermediate oral exposure to hexachloroethane. The MRL was derived from a NOAEL of 1 mg/kg/day in a study where HEXACHLOROETHANE 67 2. HEALTH EFFECTS groups of 10 male and 10 female rats were given hexachloroethane at 1, 15, or 65 mg/kg/day in the diet for 16 weeks (Gorzinski et al. 1985). All rats survived the 16-week exposure period and there were no clinical signs of compound toxicity. Organ weights were not significantly different than those of the controls except for absolute and relative liver weights and kidney weights of males treated at the highest dose. Swelling of the hepatocytes was present in males at the two highest doses. At the 15-mg/kg dose, swollen hepatocytes were noted in 6 of 10 males, and 8 of 10 males were affected at the 62-mg/kg/day dose. Swollen hepatocytes were seen in four control males and in three males from the lowest dose group. Hepatocyte size was not affected in females, but absolute and relative liver weights were increased in the highest dose group. The male rats exhibited renal tubular atrophy, hypertrophy, dilation, and degeneration for both the 15- and 62- mg/kg/day doses. Atrophy and tubular degeneration was also present in 6 of 10 females at the 62- mg/kg/day dose and 2 of 10 females at the 15 mg/kg/day dose. The 15 mg/kg/day dose was identified as the LOAEL in this study with the 1-mg/kg/day dose as the NOAEL. This NOAEL was used with an uncertainty factor of 100 (10 each for interspecies and intraspecies variability) to derive the MRL. Insufficient information was available to derive a chronic-duration oral exposure MRL for hexachloroethane. Death. No studies were located regarding lethality in humans after exposure to hexachloroethane. LD, values for animals range from 4,460 to 5,160 mg/kg when hexachloroethane is administered by gavage in corn oil and from 7,080 to 7,690 mg/kg when administered in an aqueous methyl cellulose solution (Weeks et al. 1979). The higher LD, value for the aqueous solution indicates that absorption from this medium is lower than from a digestible food oil. When exposures occurred by the inhalation route, 1 of 6 rats died during an 8-hour exposure to 5,900 ppm (Weeks et al. 1979). At this concentration, the inhalation chamber contained crystalline hexachloroethane as well as hexachloroethane vapors. The dermal LD,, was greater than 32,000 mg/kg when hexachloroethane was applied to shaved rabbit skin for 24 hours (Weeks et al. 1979). This suggests poor dermal absorption of hexachloroethane and agrees with a calculated low dermal absorption rate of 0.023 mg/cm? hr based on physical properties (Fiserova- Bergerova et al. 1990). HEXACHLOROETHANE 68 2. HEALTH EFFECTS There were some deaths among dogs, rats, and guinea pigs with exposure to 260 ppm in air for 6 weeks (Weeks et al. 1979). Following oral exposure, death occurred in rats at doses of 750 mg/kg/day (NTP 1989) and in mice at doses of 1,780 mg/kg/day (NTP 1977). Lower doses were nonlethal. Chronic oral exposure to 212 mg/kg/day shortened the life expectancy of male and female rats (NTP 1977), but doses of 20 mg/kg/day in males and 160 mg/kg/day in females did not (NTP 1989). Although mice were exposed to oral doses of 590 and 1,170 mg/kg/day hexachloroethane for 78 weeks, poor survival among male controls made it difficult to evaluate the effects of hexachloroethane. Survival for the high-dose females was slightly less than that for vehicle controls, but the differences were not significant (NTP 1977). LDy, values and the lowest lethal doses for acute- and intermediate-duration exposures classify hexachloroethane as slightly toxic (Hodge and Sterner 1949). It is unlikely that exposures to hexachloroethane at levels found at hazardous waste sites would cause death in humans. Systemic Effects There are no data for cardiovascular, gastrointestinal, musculoskeletal, endocrine, or ocular effects in humans following exposure to hexachloroethane by any route. Data are available for inhalation and oral exposures in several animal species. The only available dermal exposure data apply to dermal and ocular effects. Respiratory Effects. Pulmonary function tests were not affected in workers exposed to hexachloroethane for 5 weeks while wearing protective equipment (Selden et al. 1994). Acute exposure of rats to 5,900 ppm hexachloroethane (a combination of gaseous and microcrystalline material) resulted in interstitial pulmonary pneumonitis (Weeks et al. 1979). These pulmonary lesions were seen after a 14-day recovery period. The entrapment of solid hexachloroethane particles in the lungs could have contributed to the symptoms observed. Excess mucus in the nasal turbinates, irritation of the epithelium, and increased incidence of a mycoplasma respiratory infection were seen in rats with inhalation exposure to 260 ppm for 6 weeks and in pregnant rats with inhalation exposure to 48 ppm for 11 days. Pulmonary irritation was also present in pregnant rats treated with an oral dose of 500 mg/kg/day for 11 days (Weeks et al. 1979). Effects on the respiratory HEXACHLOROETHANE 69 2. HEALTH EFFECTS epithelium were not apparent in the tissue of the lungs, nasal cavity, nasal turbinates, larynx, trachea, or bronchi based on histopathological examination (NTP 1977, 1989; Weeks et al. 1979). Exposure to hexachloroethane, especially in its vaporous state, may weaken the effectiveness of respiratory tract mucus as an antimicrobial barrier and, thus, increase the incidence of pulmonary infections in exposed animals. Alternatively, it may weaken disease resistance by some other mechanism. Humans exposed to hexachloroethane vapors in the environment could experience an increased risk of respiratory tract infections. Cardiovascular Effects. There were no histopathological effects on the heart after inhalation or oral exposure at any concentration tested (15-5,900 ppm for the inhalation route and 1-750 mg/kg/day for the oral route) and with acute, intermediate, or chronic exposure durations (Gorzinski et al. 1985; NTP 1977, 1989; Weeks et al. 1979). The risk that humans will experience adverse effects on the cardiovascular system as the result of exposure to hexachloroethane through the environment seems to be relatively low. Gastrointestinal Effects. There were no histopathological effects on the stomach, small intestines, or large intestines with inhalation or oral exposure to hexachloroethane at any concentration tested (15-5,900 ppm for the inhalation route and 1-750 mg/kg/day for the oral route) and with acute, intermediate, or chronic exposure durations (Gorzinski et al. 1985; NTP 1977, 1989; Weeks et al. 1979). The risk that humans will experience adverse effects on the gastrointestinal system as the result of exposure to hexachloroethane in the environment seems to be relatively low. Hematological Effects. Routine blood parameters (hemoglobin, erythrocyte, leukocyte and thrombocyte levels) measured in 11 hexachloroethane-exposed workers who wore protective clothing did not differ from those of the controls (Selden et al. 1994). Hexachloroethane plasma levels in these workers were 7.3 + 6 pg/L (Selden et al. 1993). The effects of acute exposures to hexachloroethane on hematological parameters were not evaluated in animals. Inhalation doses of 260 ppm for 6 weeks had no effect on erythrocyte counts in dogs (Weeks et al. 1979) and oral exposures of up to 62 mg/kg/day for 16 weeks had no effect on red cell counts, hemoglobin concentrations, or white cell counts in rats (Gorzinski et al. 1985). These results suggest that hexachloroethane does not affect hematological parameters, but there are relatively few data upon which to base this conclusion. On the basis of the existing data, the occurrence of hexachloroethane at hazardous waste sites should not pose a significant hematological risk for humans. HEXACHLOROETHANE 70 2. HEALTH EFFECTS Musculoskeletal Effects. Neither inhalation nor oral exposures to hexachloroethane were associated with histopathological changes in skeletal muscle or bone in rats following acute-, intermediate-, or chronic- duration exposures with inhalation exposure concentrations of 15-5,900 ppm or oral exposure doses of 1-750 mg/kg/day (Gorzinski et al. 1985; NTP 1977, 1989; Weeks et al. 1979). More comprehensive data pertaining to the musculoskeletal system were not identified. Based on the data available, there appears to be no risk for musculoskeletal effects for those who live or work near a hazardous waste site. Hepatic Effects. Liver function tests (serum bilirubin, alkaline phosphatase, alanine aminotransferase, aspartate aminotransferase, gamma-glutamyl transferase) were not affected in 11 hexachloroethane- exposed workers who wore protective clothing (Selden et al. 1993). Animal studies indicate that hepatic tissues are moderately vulnerable to exposure to hexachloroethane especially when exposure occurs by the oral route. With acute- and intermediate-duration inhalation exposures, the only effects noted were an increase in liver weight in rats and guinea pigs, but not dogs or quail, after 6 weeks of exposure to 260 ppm (Weeks et al. 1979). There were no observable histopathological changes in the tissues that accompanied the organ weight change and no histopathological changes with acute exposure to an even higher hexachloroethane concentration (5,900 ppm). When exposures occurred by the oral route, increased liver wei ghts, increases in serum liver enzyme levels, centrilobular necrosis, fatty degeneration, hemosiderin-laden macrophages, and hemorrhage were noted in animals following acute- and intermediate-duration exposures (Fowler 1969b; Gorzinski et al. 1985; NTP 1989; Weeks et al. 1979). The lowest LOAEL for these effects was a dietary dose of 15 mg/kg/day for 16 weeks which was associated with enlargement of the hepatocytes in males (Gorzinski etal. 1985). However, there were no observable adverse effects on tissue histopathology in male rats given 20 mg/kg/day for 2 years or in females given 160 mg/kg/day for the same period of time (NTP 1989). Organ weights were not determined for the chronic exposures. These data suggest that there is a potential for individuals who might be exposed to hexachloroethane from a contaminated drinking water supply to experience hepatic effects. The risk from other exposure routes (inhalation or dermal) due to contaminated hazardous waste sites is probably minimal. HEXACHLOROETHANE 71 2. HEALTH EFFECTS Renal Effects. No effects on renal function tests (serum creatinine and urate, urinary hemoglobin, protein and glucose) were noted in 11 hexachloroethane-exposed workers who wore protective clothing (Selden et al. 1994). Acute exposure to concentrations of 260-5,900 ppm hexachloroethane had minimal effects on the kidney. There was an increase in kidney weights in male rats exposed to 260 ppm hexachloroethane for 6 weeks but no discernable effects on tissue histopathology (Weeks et al. 1979). This same exposure concentration had no effect on female rats or on male or female dogs, guinea pigs, or quail under parallel exposure conditions. Acute-, intermediate-, and chronic-duration oral exposures of male rats to doses of 10 mg/kg/day or greater were associated with renal tubular nephropathy (Gorzinski et al. 1985; NTP 1977, 1989; Weeks et al. 1979). Affected animals displayed tubular necrosis, hyaline droplets in tubular epithelial cells, regenerative tubular epithelium, interstitial nephritis, and fibrosis. The severity of the renal lesions varied with the dose and the duration of exposure. Hexachloroethane is a member of a family of compounds that bind to the male rat excretory protein a2p-globulin and form hyaline droplets in the tubular epithelium leading to necrosis and repair hyperplasia (Borghoff 1993; Olson et al. 1990). The hexachloroethane metabolites tetrachloroethene and pentachloroethane are also members of this family of compounds (Borghoff 1993; Swenberg 1993). Female rats and laboratory animals from other species synthesize only minimal quantities of this protein and, thus, have a lower risk for renal effects. In male rats, «2u-globulin accounts for 26% of the urinary protein, and chemicals that bind with it have a strong tendency to accumulate in the kidney causing cellular damage. Mild to moderate nephropathy in female rats exposed to 80 or 160 mg/kg/day for 2 years, a high incidence of nephropathy in mice exposed to 590 or 1,179 mg/kg/day for 78 weeks, and nephrosis in rabbits exposed to 320 or 1,000 mg/kg/day for 12 days, indicate that hexachloroethane has an effect on the kidney that is independent of a2p-globulin (NTP 1977, 1989; Weeks et al. 1979). Thus, the public health risk for renal effects should be considered when evaluating the possible effects of human exposure to hexachloroethane at hazardous waste sites. HEXACHLOROETHANE 72 2. HEALTH EFFECTS Endocrine Effects. Histological changes have not been observed in the pancreas or adrenal glands of rats, guinea pigs, dogs, or quail following inhalation exposure to hexachloroethane at concentrations up to 260 ppm for 6 weeks (Weeks et al. 1979). Intermediate-duration oral treatment of rats with hexachloroethane at doses up to 62 mg/kg/day also did not result in histological changes in the pancreas, adrenal glands, thyroid, or parathyroid glands (Gorzinski et al. 1985). Chronic gavage treatment of male rats with hexachloroethane at 10 or 20 mg/kg/day did result in an increased incidence of pheochromocytomas in the adrenal gland (NTP 1989). The relevance of this effect to humans is not clear. Dermal Effects. Hexachloroethane-exposed workers reported a slightly higher prevalence of dry skin and dry mucous membranes as well as itching and other skin problems than the unexposed controls (Selden et al. 1994). Clinical examinations of the 11 exposed workers did not reveal signs of abnormal dermatological status. The investigators indicate that the dermal effects may also have been a result of a local trauma effect of the protective equipment. There was no evidence that crystalline hexachloroethane affected the skin of animals with either inhalation or oral exposures of acute, intermediate, or chronic durations (Fowler 1969b; Gorzinski et al. 1985; NTP 1977, 1989; Weeks et al. 1979). When a water paste was placed on the shaved skin of rabbits for 24 hours, there was only a slight redness as the result of contact (Weeks et al. 1979). The concentrations of hexachloroethane that might be found at hazardous waste sites are unlikely to act as skin irritants in humans. Ocular Effects. Inhalation and oral exposure of animals to hexachloroethane caused lacrimation and reddening of the eyes after oral exposure (NTP 1977, 1989), or closing of the eyes as an avoidance mechanism during inhalation exposure (Weeks et al. 1979). Overnight, direct contact of the eyes with crystalline hexachloroethane resulted in corneal opacity and iritis in rabbits, but recovery was complete 3 days later (Weeks et al. 1979). Direct eye contact with hexachloroethane at hazardous waste sites may result in an eye irritation. Body Weight Effects. Decreased weight gains occurred in rats in response to both acute inhalation exposure to a high concentration of hexachloroethane (5,900 ppm) and intermediate-duration exposures to a lower concentration (260 ppm) (Weeks et al. 1979). Oral exposures were also associated with decreased weight gains with doses of 320 mg/kg/day or greater for 12 days in rabbits (Weeks et al. 1979) and with HEXACHLOROETHANE 73 2. HEALTH EFFECTS 562 mg/kg/day or greater for 6-16 weeks in rats (NTP 1977, 1989). Female rats exposed to 750 mg/kg/day for 16 days actually lost 25% of their initial body weight (NTP 1989). Decreased weight gain occurred in mice at doses of 1,760 mg/kg/day (NTP 1977). In light of these findings, the concentrations of hexachloroethane found at hazardous waste sites are unlikely to be of great enough magnitude to have an effect on body weight in humans. Immunological and Lymphoreticular Effects. No studies were located regarding immunological effects in humans after exposure to hexachloroethane. In addition, there were no data from comprehensive studies of immune response in animals for exposure by any route and for any duration. When the tissue histopathology of the spleen, thymus, and, in one case, lymph nodes were evaluated, no abnormalities were noted (Gorzinski et al. 1985; NTP 1989; Weeks et al. 1979). After 6-week inhalation exposures to 260 ppm hexachloroethane, the relative spleen weight was increased in young, but not in older, male rats. Data on dermal sensitization in guinea pigs indicate that exposure to low levels of hexachloroethane does not elicit antibody formation leading to an allergic dermatological response (Weeks et al. 1979). An increased incidence in mycoplasma infections in rats exposed to 260 ppm hexachloroethane for 6 weeks suggests that hexachloroethane might weaken resistance to infection (Weeks et al. 1979). This could be the result of either a change in the quantity or consistency of the respiratory tract mucus or a systemic weakening of the immune system. The data are inadequate to formulate any hypothesis regarding the mechanism for diminished host resistance or to postulate whether hexachloroethane in the environment might lower the resistance of humans to respiratory infections. Neurological Effects. No studies were located regarding neurological effects in humans after exposure to hexachloroethane. Inhalation, oral, and dermal exposure of animals to moderate or high doses (260 ppm, 5,900 ppm, 375 mg/kg/day, 750 mg/kg/day) resulted in hyperactivity, tremors, fasciculation of the facial muscles, ataxia, convulsions, and/or prostration (Fowler 1969b; NTP 1977, 1989; Southcott 1951; Weeks et al. 1979). Reduced motor activity has also been observed following oral exposure of pregnant rats (167 mg/kg/day) (Shimizu et al. 1992). Inhalation exposure of rats to 260 ppm for 6 weeks did not have any effect on spontaneous motor activity or shock avoidance behavior (Weeks et al. 1979). Ataxia, tremors, and prostration in sheep given hexachloroethane (170 or 338 mg/kg) for a liver fluke infection were successfully ameliorated with calcium as calcium borogluconate. This suggests that the neurological action of hexachloroethane may be the result of interference with the availability of calcium HEXACHLOROETHANE 74 2. HEALTH EFFECTS within excitable cells. This mechanism would explain the transient nature of the hexachloroethane neurotoxicity and is compatible with the low affinity that hexachloroethane shows for brain tissue (Fowler 1969b). There were no effects at any of the doses tested on the histopathology of the brain for any duration or route of exposure (Gorzinski et al. 1985; NTP 1977, 1989; Weeks et al. 1979). This observation is consistent with tissue distribution studies which indicate that hexachloroethane has no particular affinity for the brain tissues (Fowler 1969b). Based on the available data, the concentrations of hexachloroethane at hazardous waste sites are unlikely to reach levels that would elicit a neurological response in humans. However, there have not been any comprehensive studies of brain or nerve function after exposure to hexachloroethane. Reproductive Effects. No studies of reproductive effects in humans were located. In animals, hexachloroethane adversely affected fertility following oral exposure, but no effects were reported following inhalation exposure (Weeks et al. 1979). The absence of quantitative data on reproductive parameters, as well as evaluation of parameters that are pertinent to the assessment of reproductive risk, precludes any meaningful determination of the potential for hexachloroethane to cause adverse effects on human reproduction. Developmental Effects. No studies were located regarding the developmental effects of hexachloroethane in humans. Fetal body weights were reduced, late-gestation resorptions were increased, and the degree of ossification was reduced in offspring from pregnant rats treated orally with hexachloroethane at 500 mg/kg/day on gestation days 7-17 (Shimizu et al. 1992) or gestation days 6-16 (Weeks et al. 1979). The 500-mg/kg/day dose also caused a significant decrease in maternal body weights. No effect on the number of fetuses with anomalies was observed, and no fetal or maternal effects were observed at lower doses. These studies suggest that in the absence of maternal effects, developmental effects in humans are unlikely. Genotoxic Effects. No studies were located regarding the genotoxic effects of hexachloroethane in humans after inhalation, oral, or dermal exposure. In vitro studies of hexachloroethane using microbial, fungal, and rodent cell assays are summarized in Table 2-4. Tests of prokaryotic cell systems failed to detect gene mutation (Haworth et al. 1983; Roldan-Arjona et al. 1991; Simmon and Kauhanen 1978; TABLE 2-4. Genotoxicity of Hexachloroethane In Vitro Results With Without Species (test system) End point activation activation Reference Prokaryotic organisms: Salmonella typhimurium (TA98, Gene mutation - - Haworth et al. 1983 TA100, TA1535, TA1537) S. typhimurium (TA98, TA100, Gene mutation - - Weeks et al. 1979 TA1535, TA1537, TA1538) S. typhimurium (BA13) Gene mutation — - Roldan-Arijona et al. 1991 S. typhimurium (TA98, TA100, Gene mutation - - Simmon and Kauhanen TA1535, TA1537, TA1538) 1978 S. typhimurium (TA1535/psk1002) DNA damage - - Nakamura et al. 1987 Eukaryotic organisms: Fungi: Saccharomyces cerevisiae D, Gene mutation - - Weeks et al. 1979 S. cerevisiae D, DNA damage/repair — - Simmon and Kauhanen 1978 S. cerevisiae Gene mutation - - Bronzetti et al. 1989 Aspergillus nidulans diploid Chromosomal abberation - Not tested Crebelli et al. 1988 strains P1 Mammalian cells: Chinese hamster ovary Chromosomal aberration - - Galloway et al. 1987 Chinese hamster ovary Sister chromatid exchange + — Galloway et al. 1987 Mouse (Balb/C-3T3) Cell transformation Not tested - Tu et al. 1985 — = negative result; + = positive result; DNA = deoxyribonucleic acid S103443 H1TV3H ¢ INVHLIOHOTHOVX3IH SL HEXACHLOROETHANE 76 2. HEALTH EFFECTS Weeks et al. 1979) or DNA damage (Nakamura et al. 1987) following hexachloroethane treatment. Similar results were reported for eukaryotic cells. Hexachloroethane did not cause gene mutation in cells harvested from the stationary growth phase (Bronzetti et al. 1989) or DNA damage in yeast (Saccharomyces cerevisiae) (Simmon and Kauhanen 1978), chromosomal aberrations in fungi (Aspergillus nidulans) (Crebelli et al. 1988), chromosomal aberrations in Chinese hamster ovary cells (Galloway et al. 1987), or cell transformations in mouse cells (Tu et al. 1985). Hexachloroethane did cause sister chromatid exchanges in Chinese hamster ovary cells in the presence of activation; however, the overall importance of this response is reduced since these effects occurred at doses that were cytotoxic (e.g., induced cell cycle delay) (Galloway et al. 1987). Similarly, hexachloroethane induced a significant (p<0.01) increase of gene conversion in S. cerevisiae cells harvested from the logarithmic growth phase. Similar effects were not seen in stationary growth phase cells, both with and without metabolic activation (Bronzetti et al. 1989). Because cells of this sort contain a high level of cytochrome P-450, it is plausible that the positive responses were due to metabolites rather than the parent compound. Cancer. Only one report was located regarding an association between hexachloroethane and cancer in humans (Selden et al. 1989). In this study a liver tumor was found in an adult male who had used a product containing hexachloroethane at work for 6 years. However, under the conditions of use, the hexachloroethane reacted to form hexachlorobenzene and other chlorinated compounds which were as likely, or more likely, to have contributed to the tumorigenesis as the hexachloroethane. Lifetime exposure of rats to hexachloroethane resulted in renal carcinomas and adenomas in Fischer-344 male rats (NTP 1989). The incidence of adenomas was 1/50 for the controls, 2/50 for animals at a dose of 10 mg/kg/day, and 4/50 for animals at a dose of 20 mg/kg/day. In the animals from the high-dose group, there were also 3/50 renal carcinomas. The number of tumors (carcinomas and adenomas) was significantly greater in exposed rats than in both controls and historical controls using the Fisher Exact Test (NTP 1989). No tumors were seen in the female rats. In an earlier study, there were renal tubular cell adenomas in 5/50 Osborne-Mendel rats receiving doses of 212 mg/kg/day but no tumors in 49 animals receiving 423 mg/kg/day or in 20 vehicle control rats (Weisburger 1977). Despite the lack of tumors, there was a high incidence of nephropathy (18-66%) in exposed male and female rats. HEXACHLOROETHANE 77 2. HEALTH EFFECTS The male rat kidney is susceptible to the induction of tumors because of a2u-globulin excretion (Borghoff 1993; Olson et al. 1990). This protein is not made by female rats, other laboratory species, or humans in significant quantities, but large amounts are synthesized and excreted by male rats. EPA (1991a) has concluded that renal tumors in male rats that are associated with a2p-globulin should not be used in assessing the potential for any chemical to cause renal tumors in humans. Compounds that bind to a2p-globulin lead to the formation of hyaline droplets in the kidney causing cell damage and regenerative hyperplasia (Borghoff 1993; Olson et al. 1990). A statistically significant increase in hepatocellular carcinomas was seen in male and female mice that were dosed with 590 and 1,179 mg/kg/day hexachloroethane in corn oil by gavage for 78 continu- ous weeks (Weisburger 1977). The incidence of tumors in the exposed mice was greater than that in controls on the basis of both the Fisher Exact test and the Cochran-Armitage test. There were no hepatic tumors in male or female rats with chronic exposure to doses of 10-423 mg/kg/day (NTP 1977, 1989; Weisburger 1977). Hexachloroethane may function as a promoter rather than an inducer of hepatic tumors. When male rats were given a single dose of 497 mg/kg hexachloroethane followed by daily treatment with a known promotor (phenobarbital) for 7 weeks, there was no increase in the number of GGT+ foci in the liver (Milman et al. 1988). GGT+ foci are markers for precarcinogenic cell changes. When a single dose of a known initiator dimethylnitrosamine was followed by 7 weeks of dosing with 497 mg/kg/day hexachloroethane, the number of GGT+ foci was four times the number seen with a single dose of dimethyInitrosamine in the absence of hexachloroethane treatment. The fact that hexachloroethane does not appear to be mutagenic in short-term tests of genetic toxicity and that it has a low tendency to bind to DNA (Lattanzi et al. 1988) is consistent with classifying it as a promotor rather than a direct acting carcinogen. NTP determined that there was clear evidence of carcinogenicity in male rats based on the increased incidence of renal neoplasms and no evidence of carcinogenic activity in female rats (NTP 1989). The EPA classified hexachloroethane as a possible human carcinogen (Group C). The slope factor calculated by EPA is 1.4x10 (mg/kg/day) for both the oral and inhalation routes of exposure (IRIS 1995). IARC has determined that hexachloroethane is not classifiable as to human carcinogenicity (Group 3). HEXACHLOROETHANE 78 2. HEALTH EFFECTS 2.6 BIOMARKERS OF EXPOSURE AND EFFECT Biomarkers are broadly defined as indicators signaling events in biologic systems or samples. They have been classified as markers of exposure, markers of effect, and markers of susceptibility (NAS/NRC 1989). Due to a nascent understanding of the use and interpretation of biomarkers, implementation of biomarkers as tools of exposure in the general population is very limited. A biomarker of exposure is a xenobiotic substance or its metabolite(s), or the product of an interaction between a xenobiotic agent and some target molecule(s) or cell(s) that is measured within a compartment of an organism (NAS/NRC 1989). The preferred biomarkers of exposure are generally the substance itself or substance-specific metabolites in readily obtainable body fluid(s) or excreta. However, several factors can confound the use and interpretation of biomarkers of exposure. The body burden of a substance may be the result of exposures from more than one source. The substance being measured may be a metabolite of another xenobiotic substance (e.g., high urinary levels of phenol can result from exposure to several different aromatic compounds). Depending on the properties of the substance (e.g., biologic half-life) and environmental conditions (e.g., duration and route of exposure), the substance and all of its metabolites may have left the body by the time samples can be taken. It may be difficult to identify individuals exposed to hazardous substances that are commonly found in body tissues and fluids (e.g., essential mineral nutrients such as copper, zinc, and selenium). Biomarkers of exposure to hexachloroethane are discussed in Section 2.6.1. Biomarkers of effect are defined as any measurable biochemical, physiologic, or other alteration within an organism that, depending on magnitude, can be recognized as an established or potential health impairment or disease (NAS/NRC 1989). This definition encompasses biochemical or cellular signals of tissue dysfunction (e.g., increased liver enzyme activity or pathologic changes in female genital epithelial cells), as well as physiologic signs of dysfunction such as increased blood pressure or decreased lung capacity. Note that these markers are not often substance specific. They also may not be directly adverse, but can indicate potential health impairment (e.g., DNA adducts). Biomarkers of effects caused by hexachloroethane are discussed in Section 2.6.2. A biomarker of susceptibility is an indicator of an inherent or acquired limitation of an organism's ability to respond to the challenge of exposure to a specific xenobiotic substance. It can be an intrinsic genetic or other characteristic or a preexisting disease that results in an increase in absorbed dose, a decrease in the HEXACHLOROETHANE 79 2. HEALTH EFFECTS biologically effective dose, or a target tissue response. If biomarkers of susceptibility exist, they are discussed in Section 2.8, "Populations That Are Unusually Susceptible." 2.6.1 Biomarkers Used to Identify or Quantify Exposure to Hexachloroethane Based on results from animal studies, urinary and fecal excretion of hexachloroethane can be used to identify recent exposures (Fowler 1969b; Jondorf et al. 1957). Recent exposure to hexachloroethane can also be determined by measuring the amount of hexachloroethane in the blood, but this would be a more invasive procedure than analyzing urine or fecal matter (Fowler 1969b). The concentrations of hexachloroethane in fecal matter were higher than those in urine in sheep for the 24-hour period following exposure (Fowler 1969b). Thus, fecal matter might be better for analysis than urine. Both hexachloroethane and its lipophilic metabolites can distribute to body fat. Only hexachloroethane can be used to confirm compound exposure by way of a fat biopsy, since some of its metabolites are also produced from other chlorinated hydrocarbons or are present as contaminants in the environment. Based on one worker occupationally exposed to hexachloroethane, Selden et al. (1993) estimated that the plasma half-life in humans was several days, but less than one week. A clearance half-life in rats of 2.5 days was reported for hexachloroethane absorbed from the diet (Gorzinski et al. 1985). Therefore, similar to measurement of hexachloroethane in blood, urine, and feces, hexachloroethane in body fat is representative of current exposures rather than exposures that occurred weeks or months before testing. 2.6.2 Biomarkers Used to Characterize Effects Caused by Hexachloroethane No information was located regarding adverse health effects of hexachloroethane in humans; therefore, no judgment can be made concerning possible biomarkers of exposure in humans. Animal data suggest that renal and liver effects may occur in humans exposed to high doses of hexachloroethane. Kidney and liver effects are not specific to hexachloroethane. Lesions of the kidney (nephropathy, linear mineralization, and hyperplasia) were reported at 10 mg/kg/day or greater in male rats (NTP 1989). Urinalysis also revealed granular and cellular casts in rats exposed to hexachloroethane (47 mg/kg/day or greater) for 13 weeks (NTP 1989). Because other compounds cause similar effects and because some of these effects are unique to male rats, they are not valuable as biomarkers for human hexachloroethane exposure. HEXACHLOROETHANE 80 2. HEALTH EFFECTS The liver is also a target of hexachloroethane toxicity, but the effects are not as severe as for the kidneys. For the most part, effects in rats were confined to swelling of hepatocytes which occurred at dose levels of 15 mg/kg/day or greater following oral exposure (Gorzinski et al. 1985). Certain biochemical parameters that are commonly associated with chemically-induced liver damage were assessed in rabbits exposed to hexachloroethane by gavage for 12 days (Weeks et al. 1979) and in sheep given a single dose of 500 mg/kg (Fowler 1969b). There were no statistically significant alterations in serum enzymes (alanine amino transferase, aspartate aminotransferase, and alkaline phosphatase) or bilirubin in rabbits, but serum values were increased as compared to controls (Weeks et al. 1979). Plasma sorbitol dehydrogenase, glutamate dehydrogenase, and ornithine carbamoyl transferase concentrations increased in sheep (Fowler 1969b). Because these effects can also be caused by other chemicals, they cannot be considered specific biomarkers for hexachloroethane. 2.7 INTERACTIONS WITH OTHER SUBSTANCES Hexachloroethane is commonly used by the military for pyrotechnics and smoke screens. Hexachloroethane-containing, smoke-producing devices combine hexachloroethane with zinc oxide (Gordon et al. 1991). Small quantities of other materials such as calcium silicide can also be present. Hexachloroethane is generally about 44-47% of the reaction mixture. When a smoke pot or grenade is ignited, hexachloroethane reacts with zinc oxide to produce zinc chloride. Only small amounts (0.3-5%) of hexachloroethane remain. Other products of the reaction are tetrachloroethylene, carbon tetrachloride, phosgene, and hexachlorobenzene (Gordon et al. 1991). The environmental residues from smoke generation vary with the configuration of the device and its position when it ignites (upright or prone) (Schaeffer et al. 1988). A number of studies of the toxicity of zinc oxide/hexachloroethane smoke have been conducted (Brown et al. 1990; Karlsson et al. 1986; Marrs et al. 1983). These studies demonstrate that smoke exposure results in pulmonary inflammation and irritation. When male Porton Wistar rats were exposed to hexachloroethane/zinc oxide smoke for 60 minutes, the lungs showed pulmonary edema, alveolitis, and areas of macrophage infiltration 3 days later. At 14 days, there was interstitial fibrosis and macrophage infiltration. At 28 days, increased fibrosis and macrophage infiltration were noted. However, these same symptoms occurred when the animals inhaled zinc chloride; there was no apparent synergism between the zinc chloride and residual hexachloroethane (Brown et al. 1990; Richard et al. 1989). This is consistent HEXACHLOROETHANE 81 2. HEALTH EFFECTS with the fact that smoke contains little hexachloroethane and the observation that acute exposure to 260 ppm hexachloroethane had no effects on the lungs of rats (Weeks et al. 1979). Environmental agents that influence microsomal reactions will influence hexachloroethane toxicity. The production of tetrachloroethene as a metabolite is increased by agents like phenobarbital that induce certain cytochrome P-450 isozymes (Nastainczyk et al. 1982a; Thompson et al. 1984). Exposure to food material or other xenobiotics that influence the availability of mixed function oxidase enzymes and/or cofactors will change the reaction rate and end products of hexachloroethane metabolism and thus influence its toxicity. No other studies of interactions of hexachloroethane with other chemicals were identified in the published literature. However, the primary metabolites of hexachloroethane (tetrachloroethene and pentachloroethane) are themselves toxic and would be expected to exacerbate hexachloroethane toxicity if they were present in a mixture with hexachloroethane. Concurrent carbon tetrachloride exposure would also be expected to exacerbate hexachloroethane toxicity. Both hexachloroethane and carbon tetrachloride are processed by microsomes to generate free radicals, and carbon tetrachloride also forms endogenous hexachloroethane in the liver (Fowler 1969a). 2.8 POPULATIONS THAT ARE UNUSUALLY SUSCEPTIBLE A susceptible population will exhibit a different or enhanced response to hexachloroethane than will most persons exposed to the same level of hexachloroethane in the environment. Reasons include genetic make-up, developmental stage, age, health and nutritional status (including dietary habits that may increase susceptibility, such as inconsistent diets or nutritional deficiencies), and substance exposure history (including smoking). These parameters may result in decreased function of the detoxification and excretory processes (mainly hepatic, renal, and respiratory) or the pre-existing compromised function of target organs (including effects or clearance rates and any resulting end-product metabolites). For these reasons we expect the elderly with declining organ function and the youngest of the population with immature and developing organs will generally be more vulnerable to toxic substances than healthy adults. Populations who are at greater risk due to their unusually high exposure are discussed in Section 5.6, "Populations With Potentially High Exposure." HEXACHLOROETHANE 82 2. HEALTH EFFECTS No studies were located regarding populations that are unusually susceptible to hexachloroethane toxicity. Because the kidney and liver are the primary target tissues, individuals with compromised liver or kidney function would have an increased risk from exposure. Susceptibility to pulmonary infections could be increased by exposure to hexachloroethane vapors and, thus, individuals that suffer from chronic respiratory problems could also have an increased risk from hexachloroethane exposure. The risk to overweight individuals consuming a high fat diet is likely to be greater than that for lean individuals. Excess deposits of body fat increase physiological exposure durations due to the affinity of the adipose tissue for hexachloroethane. Hexachloroethane collects in the adipose deposits during exposure and is released slowly to circulatory fluids after the exposure has ceased. Individuals consuming a high fat diet are likely to absorb increased quantities of hexachloroethane when exposure occurs through the oral route; absorption from a lipid matrix is favored over absorption from an aqueous medium. 2.9 METHODS FOR REDUCING TOXIC EFFECTS This section describes clinical practice and research concerning methods for reducing toxic effects of exposure to hexachloroethane. However, because some of the treatments discussed may be experimental and unproven, this section should not be used as a guide for treatment of exposures to hexachloroethane. When specific exposures have occurred, poison control centers and medical toxicologists should be consulted for medical advice. 2.9.1 Reducing Peak Absorption Following Exposure Humans can be exposed to hexachloroethane by inhalation, ingestion, or skin contact. There are no specific treatments for hexachloroethane overexposure. However, treatments available for halogenated hydrocarbons may be useful. When individuals have been exposed to vapors of hexachloroethane, they should be moved to fresh air. Additional treatment with oxygen may be beneficial. If hexachloroethane has been ingested, treatments designed to minimize absorption of halogenated hydrocarbons are appropriate. If the victim is alert, can swallow, and appears to have a good gag reflex, water (1-2 glasses) may be administered after ingestion of small amounts of hexachloroethane (Bronstein HEXACHLOROETHANE 83 2. HEALTH EFFECTS and Currance 1988; Stutz and Ulin 1992). Because many hydrocarbons may cause spontaneous vomiting, induced emesis is not recommended since it may result in aspiration of gastric contents. If large amounts of hexachloroethane have been ingested, gastric lavage may be useful if performed soon after exposure. Activated charcoal can be administered to bind hexachloroethane in the gastrointestinal tract and minimize absorption. Activated charcoal can be combined with cathartics to speed fecal excretion. Because hexachloroethane is lipid soluble, the administration of a fat-based substance or whole milk are not recommended as they may cause increased absorption. In order to minimize absorption through the skin, all contaminated clothing should be removed and the skin should be washed with mild soap and water (Bronstein and Currance 1988; Stutz and Ulin 1992). In cases where the compound has been splashed into the eyes, irrigation with large amounts of water for 15-30 minutes has been recommended. 2.9.2 Reducing Body Burden Hexachloroethane that is absorbed appears rapidly in the systemic circulation. It is distributed widely throughout the body, with the highest concentration in fat and kidney and the lowest in the muscle (Fowler 1969b; Gorzinski et al. 1985). There are no specific treatments available for reducing the body burden if hexachloroethane is absorbed. Because hexachloroethane causes renal injury, hemodialysis may be useful to reduce the plasma levels of hexachloroethane should renal failure occur in exposed persons. 2.9.3 Interfering with the Mechanism of Action for Toxic Effects No information is available on the adverse health effects of hexachloroethane in humans. Animal studies revealed that hexachloroethane primarily causes liver and kidney toxicity. Effects on the nervous system and lungs have also been reported. The mechanism by which these effects are mediated is not well characterized. Reductive metabolism by cytochrome P-450 and production of a free radical intermediate have been suggested as factors in hexachloroethane-induced hepatotoxicity (Nastainczyk et al. 1982a; Thompson et al. 1984; Town and Leibman 1984). Accordingly, one possible approach may be to reduce free radical injury. To that end, oral administration of N-acetylcysteine can be used as a means of reducing free radical injury. Also, oral administration of vitamin E and vitamin C may be of value since they are free radical scavengers. HEXACHLOROETHANE 84 2. HEALTH EFFECTS The mechanism of renal toxicity is not clear. Because the spectrum of kidney lesions observed in male rats (Gorzinski et al. 1985; NTP 1989) resembled those for a2u-globulin nephropathy, hexachloroethane- induced kidney lesions may, in part, be due to hexachloroethane binding to this protein. On the other hand, renal toxicity was observed in female rats and did not present the same sequence of lesions. This suggests the effects in males may not be totally due to a:2p-globulin. Specific methods to minimize renal toxicity, based on mechanism of action, cannot be proposed at this time. 2.10 ADEQUACY OF THE DATABASE Section 104(I)(5) of CERCLA, as amended, directs the Administrator of ATSDR (in consultation with the Administrator of EPA and agencies and programs of the Public Health Service) to assess whether adequate information on the health effects of hexachloroethane is available. Where adequate information is not available, ATSDR, in conjunction with the National Toxicology Program (NTP), is required to assure the initiation of a program of research designed to determine the health effects (and techniques for developing methods to determine such health effects) of hexachloroethane. The following categories of possible data needs have been identified by a joint team of scientists from ATSDR, NTP, and EPA. They are defined as substance-specific informational needs that if met would reduce the uncertainties of human health assessment. This definition should not be interpreted to mean that all data needs discussed in this section must be filled. In the future, the identified data needs will be evaluated and prioritized, and a substance-specific research agenda will be proposed. 2.10.1 Existing Information on Health Effects of Hexachloroethane The existing data on health effects of inhalation, oral, and dermal exposure of humans and animals to hexachloroethane are summarized in Figure 2-4. The purpose of this figure is to illustrate the existing information concerning the health effects of hexachloroethane. Each dot in the figure indicates that one or more studies provide information associated with that particular effect. The dot does not necessarily imply anything about the quality of the study or studies, nor should missing information in this figure be interpreted as a "data need." A data need, as defined in ATSDR's Decision Guide for Identifying Substance-Specific Data Needs Related to Toxicological Profiles (ATSDR 1989), is substance-specific information necessary to conduct comprehensive public health assessments. Generally, ATSDR defines a data gap more broadly as any substance-specific information missing from the scientific literature. HEXACHLOROETHANE 85 2. HEALTH EFFECTS As indicated by Figure 2-4, data available on the health effects of hexachloroethane in humans is extremely sparse. A study (Selden et al. 1994) of 11 workers who wore protective equipment while being exposed to hexachloroethane for 5 weeks showed no respiratory, hematological, liver or kidney effects at plasma levels of 7.3 + 6 pg/L (Selden et al. 1993). Because of skin irritation, the investigators suggest that the principal exposure route may have been dermal, although the dermal effects may also have been a result of trauma from the protective equipment. Because of the protective equipment it is not possible to determine exposure levels. There is one case study of a liver tumor in an individual who had used a hexachloroethane-containing degassing agent in his work for a period of 6 years (Selden et al 1989). However, during use the hexachloroethane reacted to form hexachlorobenzene and small amounts of other chlorinated compounds. Exposure to hexachloroethane was minimal compared to exposure to the reaction products. There are more data available concerning the effects of hexachloroethane in animals, particularly for exposure by the inhalation and oral routes. These studies identify the liver and kidney as target organs for hexachloroethane. There have been no studies of chronic exposure by the inhalation route. Although there are some data on neurological and immunological effects, there have been no well-designed, comprehensive studies of these systems. This is also true for reproductive and developmental effects. The data are limited and there has been no comprehensive multigeneration study of reproductive processes and only two studies of developmental effects. In vivo testing for mutagenic potential has also not been conducted. The carcinogenic potential for hexachloroethane has only been evaluated for the oral route. Data for the dermal route are limited to an LD, study and data on dermal/ocular effects. A theoretical estimation of dermal transport of hexachloroethane indicated that absorption is low. 2.10.2 Identification of Data Needs Acute-Duration Exposure. No studies were located on the effects of hexachloroethane in humans after acute exposure by any route. Acute inhalation exposure in animals caused respiratory effects, staggered gait, and reduced body weight gain, but these effects occurred at a concentration that was lethal (Weeks et al. 1979). There were no histological changes or changes in organ weights in the liver and kidneys after inhalation exposure to hexachloroethane (Weeks et al. 1979). Reproductive and HEXACHLOROETHANE 86 2. HEALTH EFFECTS FIGURE 2-4. Existing Information on Health Effects of Hexachloroethane < 2 © & AN) K SYSTEMIC = (D 8 (2) 2 &° S/F S/o S/S SE 3° SAS SSS rR © & ) & WW & FP o® ® Inhalation . ® Oral Dermal ® Human 3 2° © 2 f oO K SYSTEMIC Wo 2 N Q @ <3 o © £5 5) © i 2 £ RIAN) D>) © & 5 0 & ® & © & QW _&} & ce? oo? Inhalation | © | ® | ® eo Oral ° ® ° ° ° °® Dermal ° ® Animal ® Existing Studies HEXACHLOROETHANE 87 2. HEALTH EFFECTS developmental effects were not observed in rats exposed to hexachloroethane on gestation days 6-16 (Weeks et al. 1979). Tremors were observed at the high concentration in pregnant rats, and an acute inhalation MRL of 6 ppm was calculated based on the NOAEL for neurological effects observed in the developmental study (Weeks et al. 1979). Acute oral exposure of animals was associated with tubular nephrosis and nephrocalcinosis in the kidneys (Weeks et al. 1979), hepatocellular degeneration, coagulation necrosis, hemorrhage in the liver (Weeks et al. 1979), and elevated liver enzymes in the serum (Fowler 1969b). An MRL of 1 mg/kg was derived for acute oral exposures based on a NOAEL for the absence of liver damage in rabbits (Weeks et al. 1979). Reduced body weight gain and neurological effects (tremor, decreased motor activity) have also been observed following acute oral exposure to hexachloroethane (Shimizu et al. 1992; Weeks et al. 1979). Increased fetal resorptions, decreases in fetal body weight, and an increase in skeletal anomalies have also been observed in rats treated orally with hexachloroethane during organogenesis (Shimizu et al. 1992; Weeks et al. 1979). As the dose following inhalation exposure is limited by the amount of hexachloroethane vapor that can be formed at standard temperatures (Weeks et al. 1979), oral studies may be more useful. Additional oral exposure studies to delineate the threshold for acute liver effects and to help clarify the indices that are predictive of liver damage would be especially useful. Studies of kidney effects in female rats and other laboratory animals using the oral route would also be helpful to differentiate between lesions associated with a2u-globulin and those produced by other mechanisms. Hexachloroethane caused reversible corneal injury in rabbits following ocular contact, but contact with the skin for 24 hours resulted in no dermal effects (Weeks et al. 1979). The physical properties of hexachloroethane suggest that absorption across human skin would be limited (Fiserova-Bergerova et al. 1990). Therefore, unless dermal absorption studies indicate that this prediction is incorrect, there is no need for additional studies of acute dermal toxicity. Intermediate-Duration Exposure. A study (Selden et al. 1994) of 11 workers who wore protective equipment while being exposed to hexachloroethane for 5 weeks showed no respiratory, hematological, liver, or kidney effects at plasma levels of 7.3 + 6 ug/L (Selden et al. 1993). Because mild dermal effects were noted, the principal exposure route may have been dermal. The dermal effects may also have been a result of trauma from the protective equipment. Because of the protective equipment, it is not possible to determine exposure levels. HEXACHLOROETHANE 88 2. HEALTH EFFECTS Inhalation of 260 ppm hexachloroethane, but not 48 ppm, was associated with an increased incidence of a respiratory tract mycoplasma infection that was endemic in the rat colony (Weeks et al. 1979). Ocular irritation, reduced body weight gain, and tremors were also noted in rats at 260 ppm. Reduced body weight gain in guinea pigs and ocular irritation and tremors in dogs were noted at 260 ppm, but not 48 ppm (Weeks et al. 1979). Based on the 48 ppm concentration for the lack of neurological effects in rats (Weeks et al. 1979), an intermediate inhalation MRL of 6 ppm was calculated. Following intermediate oral exposure to hexachloroethane, decreased body weight gain has been observed in rats and mice (NTP 1977) and kidney effects, including increased kidney wei ght, tubular atrophy and hypertrophy, and hyaline droplet formation (Gorzinski et al. 1985; NTP 1989), and post-treatment hyper- activity and convulsions have been observed in rats (NTP 1989). Following intermediate exposure, liver enlargement has also been observed in rats treated with hexachloroethane (Gorzinski et al. 1985; Milman et al. 1988; Story et al. 1986). Enlargement of hepatocytes in male rats following oral exposures to 15 mg/kg/day hexachloroethane, but not 1 mg/kg/day (Gorzinski et al. 1985), was used as the basis of an MRL of 0.01 mg/kg/day for intermediate-duration oral exposures. Because there is potential for persons living near hazardous waste sites to be exposed to hexachloroethane through contaminated drinking water, additional studies of liver damage in male and female rats and kidney damage in female rats by the oral route would be useful. Hexachloroethane appears to be less bioavailable in an aqueous medium than in a lipid medium (Weeks et al. 1979). In an intermediate-duration study, dermal treatment of rats did not result in skin sensitization (Weeks et al. 1979). Additional intermediate-duration dermal studies were not available. The physical properties of hexachloroethane suggest that absorption across human skin would be limited (Fiserova-Bergerova et al. 1990). Therefore, unless dermal absorption studies indicate that this prediction is incorrect, there is no need for additional studies of intermediate dermal toxicity. Chronic-Duration Exposure and Cancer. No studies were located in humans following chronic- duration exposure to hexachloroethane for any exposure route. No chronic animal studies were conducted using the inhalation route of exposure. In oral studies with rats, the kidney was identified as a primary target organ in males and females (NTP 1989). The kidney damage in male rats was the result of hyaline droplet nephropathy and, accordingly, was not suitable as the basis for an oral MRL. In contrast to acute- and intermediate-duration oral exposure, liver toxicity was not evident in rats following chronic oral exposure. There were no studies of chronic dermal exposure to hexachloroethane. HEXACHLOROETHANE 89 2. HEALTH EFFECTS Studies using the inhalation route might be useful to determine the potential human health risk in populations that may be occupationally exposed to hexachloroethane vapors for long periods. Additional chronic oral studies may be useful to help further clarify the dose-response relationships and better characterize thresholds. Studies by the dermal route would not be useful until the rate and extent of absorption have been better characterized. The carcinogenic potential of hexachloroethane has not been evaluated following chronic inhalation or dermal exposure. Hexachloroethane increased the incidence of renal tumors in male rats (NTP 1989) following chronic oral exposure. However, these tumors were associated with renal hyaline droplets and, thus, are unique to male rats. Although kidney damage was present in female rats after lifetime exposures to 80 and 160 ppm hexachloroethane, there was no increase in renal tumors. Liver lesions and liver tumors were found in mice following long-term oral exposure (NTP 1977). A bioassay in mice (oral route) using current good laboratory practices may be useful in order to clarify whether or not hexachloroethane is a hepatic carcinogen. The suspected hepatic carcinogenicity of the hexachloroethane metabolites pentachloroethane and tetrachloroethene strengthens the justification for additional investigations of the carcinogenic potential of hexachloroethane. Studies of the mechanism of hexachloroethane carcinogenicity would also be useful to determine if effects observed in mice are applicable to humans. To further characterize risk to persons occupationally exposed to hexachloroethane, inhalation studies of the carcinogenic potential of hexachloroethane may be useful. The concentrations used in the inhalation studies would be limited to about 670-700 ppm, the saturated vapor concentration at 20°C (Weeks et al. 1979). The physical properties of hexachloroethane suggest that absorption across human skin would be limited (Fiserova-Bergerova et al. 1990). Therefore, unless dermal absorption studies indicate that this prediction is incorrect, there is no need for carcinogenic studies following dermal exposure. Genotoxicity. Hexachloroethane did not exhibit mutagenic activity in vitro in prokaryotic cells (Haworth et al. 1983; Nakamura et al. 1987, Roldan-Arjona et al. 1991; Simmon and Kauhanen 1978; Weeks et al. 1979) or in eukaryotic cells (Galloway et al. 1987; Tu et al. 1985). In vivo data from animals, such as the results of a micronucleus assay, would be of value. HEXACHLOROETHANE 90 2. HEALTH EFFECTS The mutagenic potential of hexachloroethane has not been evaluated in humans. Because hexachloroethane has been detected at hazardous waste sites, it would be useful to evaluate the potential for hexachloroethane to induce mutagenic effects in human cells (e.g., peripheral lymphocytes). Reproductive Toxicity. The effects of hexachloroethane on human reproduction have not been evaluated for any route of exposure. Data were available from animal studies using the inhalation and oral routes of exposure, but there were no data from studies using the dermal route. Following inhalation exposure to 260 ppm hexachloroethane, signs of maternal toxicity (decreased wei ght gain and clinical signs of neurotoxicity) were noted, but there was no evidence of embryotoxicity or fetotoxicity (Weeks etal. 1979). Reduced fertility, as characterized by reduced gestation indices and the number of live fetuses, occurred in pregnant rats following oral exposure during gestation (Weeks et al. 1979). Increased late-stage fetal resorptions were observed in rats treated orally with hexachloroethane at doses that resulted in maternal body weight gain 35% less than the controls (Shimizu et al. 1992). A comprehensive one- generation study focusing on a broad range of predictive parameters regarding reproductive success would be useful. Because inhalation exposure is limited by the properties of hexachloroethane, higher doses could be achieved using oral exposure. If an oral study is negative for reproductive effects at high doses, an inhalation study may not be necessary. Developmental Toxicity. No studies on developmental effects in humans using any route of exposure were located. Rats were exposed to hexachloroethane during gestation using both the oral and inhalation routes and there were no soft tissue or skeletal effects in the pups (Weeks et al. 1979). Decreased fetal body weights and delayed ossification were observed in offspring of rats treated orally with hexachloro- ethane at doses that resulted in maternal body weight gain 35% less than the controls (Shimizu et al. 1992). Malformations were not observed in either control or hexachloroethane-treated fetuses. Con- firmation of a lack of developmental effects in a second species following oral exposure would be useful. The inclusion of a developmental component to the suggested one-generation study would also provide useful data. As inhalation and dermal exposure are limited because of the physical properties of hexachloroethane that prevent exposure to high concentrations of vapor and that limit dermal absorption, studies by these routes of exposure may not be necessary. HEXACHLOROETHANE 91 2. HEALTH EFFECTS Immunotoxicity. No studies are available for any exposure route on the potential for hexachloroethane to cause immunotoxic effects in humans. Data in animals are limited to studies that evaluated lymphoid organs (e.g., spleen and thymus) as part of a comprehensive histopathological examination following oral and inhalation exposure to hexachloroethane (Gorzinski et al. 1985; Weeks et al. 1979). Adverse effects were not reported for these organs. Effects on immune function have not been evaluated in animals following any route of exposure. There was an increased frequency of pulmonary tract infections in animals following inhalation and oral exposures (Weeks et al. 1979). Responses of this sort may be due, in part, to compromised immune functions. Studies in animals, using a battery of in vitro and short-term in vivo studies of immunotoxicity following inhalation and oral exposure, may enhance our overall understanding of the effects of hexachloroethane on disease resistance. Neurotoxicity. No information is available on neurotoxic effects of hexachloroethane in humans following any route of exposure. Acute inhalation exposure in rats caused staggering gait after exposure to high concentrations (5,900 ppm) (Weeks et al. 1979). The usefulness of this data is limited since this concentration was lethal. Tremors have been reported at 260 ppm but not 48 ppm following inhalation exposure of rats in a developmental study and in a study of 6-weeks duration (Weeks et al. 1979). The lack of tremors at 48 ppm in the developmental study serves as the basis for the acute inhalation MRL, and the lack of tremors at 48 ppm in the 6-week study serves as the basis for the intermediate inhalation MRL. One study that evaluated spontaneous motor activity and avoidance behavior in rats during 6 weeks of exposure to 260 ppm hexachloroethane vapors did not reveal adverse effects of hexachloroethane on these neurobehavioral functions (Weeks et al. 1979). Acute oral doses (500 mg/kg) given to healthy sheep caused tremors of the facial muscles (Fowler 1969b); several liver-fluke-infected sheep experienced prostration with even lower doses (170 or 338 mg/kg) (Southcott 1951). Treatment of sheep with calcium relieved the clinical signs of neurotoxicity, suggesting that cellular availability of calcium ion may be related to the neuromuscular symptoms noted (Southcott 1951). Therefore, mechanistic studies of neuromuscular impulse transmission and cognitive function in animals would be useful. These neurological studies should examine the effects of different concentra- tions of hexachloroethane in several species. HEXACHLOROETHANE 92 2. HEALTH EFFECTS Postgavage hyperactivity was noted in rats with an oral dose of 375 mg/kg/day (NTP 1989) and tremors occurred following a dose of 500 mg/kg/day (Weeks et al. 1979). Other available animal data are limited to the findings of histological examination of the brain and other nervous tissue following inhalation, oral, and dermal exposures (Gorzenski et al. 1985; NTP 1977, 1989; Weeks et al. 1979). No lesions were reported. Epidemiological and Human Dosimetry Studies. No epidemiological studies of hexachloroethane exposure were identified. Epidemiological studies including endpoints such as immunotoxicity, neurotoxicity, liver enzymes, and kidney function in individuals who handle hexachloroethane in the production of military pyrotechnics and smoke-producing devices would be useful. Epidemiological studies of exposure to the hexachloroethane-generated smoke might be of little value because most of the hexachloroethane is consumed in the smoke-generating reaction. Epidemiological studies will be of greatest value when mixtures of other chlorinated hydrocarbons are not present with hexachloroethane in the occupational environment because there are similarities in metabolism and possible synergistic demands on microsomal enzymes. Biomarkers of Exposure and Effect Exposure. Hexachloroethane has been measured in the plasma of occupationally exposed humans (Selden etal. 1993). Because these workers were wearing protective equipment, it is not possible to relate exposure concentrations to plasma levels of hexachloroethane. Based on animal data, exposure to hexachloroethane can be determined by analyzing blood, urine, and fecal matter for the presence of hexachloroethane within 24 hours of exposure (Fowler 1969b). After 24 hours, most of the hexachloroethane has been metabolized to compounds that are not unique to hexachloroethane metabolism. Additional studies of biomarkers of exposure in animals are not needed at this time. Effect. No data on biomarkers of effect in humans were identified. In animals, kidney and liver effects have been reported (Fowler 1969b; Gorzinski et al. 1985 ; NTP 1989; Weeks et al. 1979). Hyaline casts were present in urine but they can be caused by other chemicals as well as hexachloroethane (Borghoff 1993). Biochemical tests (e.g., blood urea nitrogen) to detect renal damage were negative (Weeks et al. 1979). However, the usual battery of urinary tests (i.e., glucose, protein, enzymes, creatinine, electrolytes, and urine output) has not been applied. Additional studies that monitor these indices would be useful and HEXACHLOROETHANE 93 2. HEALTH EFFECTS could demonstrate whether or not hexachloroethane has an effect on glomerular filtration and/or tubular resorption. In rabbits, biochemical indices commonly used to assess liver damage (e.g., aspartate aminotransferase, alanine aminotransferase, alkaline phosphatase, bilirubin, and protein) were elevated but within normal ranges (Weeks et al. 1979). On the other hand, plasma enzyme concentrations (sorbitol dehydrogenase, glutamate dehydrogenase, and ornithine carbamoyl transferase) increased in sheep (Fowler 1969b). Because people living near hazardous waste sites are likely to be exposed for long periods, it may be useful to evaluate these parameters in hexachloroethane-exposed animals to determine if there is consistent elevation of these biomarkers of liver damage with chronic exposure. Absorption, Distribution, Metabolism, and Excretion. There are no mechanistic or quantitative studies of hexachloroethane absorption from the lungs or across the gastrointestinal tract or skin. However, absorption does occur following oral exposure based on the appearances of hexachloroethane and its metabolites in blood, urine, and exhaled air (Fowler 1969b; Gorzinski et al. 1985; Jondorf et al. 1957; Mitoma et al. 1985; Nolan and Karbowski 1978). The observation of toxic effects following inhalation exposure and dermal exposure (Weeks et al. 1979) indicates that hexachloroethane is absorbed through the respiratory tract. Quantitative studies that examine the absorption of hexachloroethane following inhalation and dermal exposure would be useful. Oral kinetic studies in rats indicate that hexachloroethane distributes preferentially to the adipose tissue (Gorzinski et al. 1985; Nolan and Karbowski 1978). Relatively high concentrations are also found in male rat kidneys (Nolan and Karbowski 1978). Moderate concentrations of hexachloroethane are found in the liver, kidneys of female rats, and blood, and small amounts in muscle, lungs, and brain (Gorzinski et al. 1985). The metabolism of hexachloroethane is relatively well defined and involves dehalogenation followed by oxidation (Fowler 1969b; Gorzinski et al. 1985; Jondorf et al. 1957; Nastainczyk et al. 1982a, 1982b; Nolan and Karbowski 1978; Salmon et al. 1981; Thompson et al. 1984; Town and Leibman 1984). Urinary by-products such as trichloroacetic acid and trichloroethanol are consistent with metabolism (Jondorf et al. 1975; Mitoma et al. 1985) and do not require additional evaluation at this time. A small portion of the exhaled radioactive label from hexachloroethane is exhaled as carbon dioxide (Mitoma et al. 1985). A more thorough investigation of the other hexachloroethane metabolites removed from the body HEXACHLOROETHANE 94 2. HEALTH EFFECTS in exhaled air would be useful, along with quantification of biliary excretion and identification of the biliary metabolites. Comparative Toxicokinetics. There are differences in the effects of hexachloroethane on different species and between sexes. Male rats are particularly susceptible to kidney damage following hexachloroethane exposure because of the binding of hexachloroethane to a2u-globulin (NTP 1989). However, nephrotoxicity is also seen in female rats and in mice and rabbits (Gorzinski et al. 1985; NTP 1977, 1989; Weeks et al. 1979) and should be examined in greater detail to identify the mechanisms for the lesions observed. Additional information on hepatic lesions in species other than the rat and mouse would be useful in evaluating the risk to humans for both noncarcinogenic and carcinogenic effects from hexachloroethane exposure. An increased risk of respiratory infections was seen in rats exposed to 260 ppm hexachloroethane for 6 weeks (Weeks et al. 1979). A similar occurrence was not noted in dogs or guinea pigs. Additional information on the susceptibility of species other than the rat to similar infections would be useful in determining the significance of this observation to human health. Comparative studies of the infection incidence should await elucidation of the mechanism for this effect. Dogs were more susceptible to neurotoxicity from hexachloroethane vapors than rats, and both species were more sensitive than guinea pigs and quail (Weeks et al. 1979). Pregnant rats were more sensitive to tremors than nonpregnant rats (Weeks et al. 1979). Once the mechanism of neurotoxicity has been determined, the advisability of examining differences in species response can be evaluated. Methods for Reducing Toxic Effects. There are no compound-specific methods for reducing the toxic effects of hexachloroethane. The mitigation procedures suggested (Bronstein and Currance 1988; Stutz and Ulin 1992) are applicable to exposure to volatile chlorinated hydrocarbons as a class and are not specific for hexachloroethane. Neither the mechanism of absorption nor the mechanism of distribution for hexachloroethane has been established. There are indications that free radical reactions may be responsible for some of the toxic effects of hexachloroethane in the liver (Town and Leibman 1984), but the data are not conclusive. When additional data on absorption, distribution and mechanism are available, compound-specific studies on methods for mitigation of toxic effects can be designed. HEXACHLOROETHANE 2. HEALTH EFFECTS 2.10.3 On-going Studies No on-going studies of the toxicity of hexachloroethane were identified. 95 HEXACHLOROETHANE 3. CHEMICAL AND PHYSICAL INFORMATION 3.1 CHEMICAL IDENTITY Table 3-1 lists common synonyms, trade names, and other pertinent identification information for hexachloroethane. 3.2 PHYSICAL AND CHEMICAL PROPERTIES Table 3-2 lists important physical and chemical properties of hexachloroethane. 97 HEXACHLOROETHANE 3. CHEMICAL AND PHYSICAL INFORMATION 98 TABLE 3-1. Chemical Identity of Hexachloroethane Characteristic Information Reference Chemical name Synonym(s) Registered trade name(s) Chemical formula Chemical structure Identification numbers: CAS registry NIOSH RTECS EPA hazardous waste OHM/TADS DOT/UN/NA/IMCO shipping HSDB NCI Hexachloroethane Perchloroethane; carbon hexachloride; 1,1,1,2,2,2- hexachloroethane; hexachloroethylene; HCE; and others Avlothane; Distokal; Distopan; Distopin; Egitol; Falkitol; Fasciolin; Mottenhexe; Phenohep C,Cl, cl cl | Cl—C—C—dl | Cl cl 67-72-1 KI 4025000 U131 No data NA 9037 2033 C04604 HSDB 1995 ACGIH 1991; Gordon et al. 1991; HSDB 1995 IARC 1979 HSDB 1995 Howard 1989 HSDB 1995 HSDB 1995 HSDB 1995 HSDB 1995 HSDB 1995 HSDB 1995 CAS = Chemical Abstracts Services; DOT/UN/NA/IMCO = Department of Transportation/United Nations/North America/International Maritime Dangerous Goods Code; EPA = Environmental Prot Hazardous Substances Data Bank; NCI = ection Agency; HSDB = National Cancer Institute; NIOSH = National Institute for Occupational Safety and Health; OHM/TADS = Oil and Hazardous Materials/Technical Assistance Data System; RTECS = Registry of Toxic Effects of Chemical Substances HEXACHLOROETHANE 3. CHEMICAL AND PHYSICAL INFORMATION 99 TABLE 3-2. Physical and Chemical Properties of Hexachloroethane Property Information Reference Molecular weight 236.74 Weast 1986 Color Colorless HSDB 1995 Physical state Solid HSDB 1995 Melting point Sublimes ACGIH 1991; Budavari Boiling point Density: at 20°C Odor Odor threshold: Water Air Solubility: Water at 22°C Water at 25°C Organic solvent(s) Partition coefficients: Log Kou Log K,. Vapor pressure: at 20°C at 30°C Henry's law constant: at 25°C: Autoignition temperature Flashpoint Flammability limits Conversion factors Explosive limits 186.8°C (triple point) 2.091 g/mL Camphoraceous 0.010 mg/L 0.15 ppm (1.5 mg/m’) 50 mg/L 14 mg/L Soluble in alcohol, benzene, chloroform, ether, oils 3.82 3.34 43 0.4 mmHg 0.8 mmHg 2.237x10? atm m*/mole 6,100 L-torr/mol (8.010 atm m*/mol 2.8x10* atm m*/mole Nonflammable Nonflammable Nonflammable | ppm = 9.68 mg/m’ 1 mg/m? = 0.10 ppm No data et al. 1989 Budavari et al. 1989 Weast 1986 Budavari et al. 1989 Amoore and Hautala 1983 Amoore and Hautala 1983 Verschueren 1983 Spanggord et al. 1985 Budavari et al. 1989 Howard 1989 Callahan et al. 1979 Mabey et al. 1982 Verschueren 1983 Verschueren 1983 Yaws et al. 1991 Spanggord et al. 1985 Howard 1989 IARC 1979 IARC 1979 IARC 1979 Verschueren 1983 HEXACHLOROETHANE 101 4. PRODUCTION, IMPORT, USE, AND DISPOSAL 4.1 PRODUCTION Hexachloroethane is usually produced commercially by the chlorination of tetrachloroethylene in the presence of ferric chloride at 100-140°C. It may also be obtained as a co-product in the production of tetrachloroethylene by pyrolysis of carbon tetrachloride at 800-900°C or by passing a mixture of ethylene and chlorine over charcoal at 300-350°C. Small amounts of high purity hexachloroethane may be prepared by the action of chlorine on barium carbide (Dacre et al. 1979; Gordon et al. 1991; IARC 1979; Santodonato et al. 1985). Hexachloroethane is not currently produced for commercial distribution in the United States. It isa by-product in the industrial chlorination of saturated and unsaturated C, hydrocarbons by several U.S. companies, including Dow Chemical, PPG Industries, and Occidental Petroleum Corporation. The product may be used captively in-house or recycled in feedstock to produce tetrachloroethylene or carbon tetrachloride. Estimates of current production volumes were not located (Gordon et al. 1991; Santodonato et al. 1985; TRI93 1995). Hexachloroethane was produced in the United States for commercial distribution from 1921 to 1967. Hummel Chemical Company, Inc., South Plainfield, New Jersey, and the Nease Chemical Company (location not provided) produced hexachloroethane at one time. In the 1970s, there were 14 producers and distributors of hexachloroethane in the United States. The producers reported that the product was not distributed; it was used in-house or recycled. The distributors were importers of hexachloroethane (see Section 4.2). Estimated production volume of hexachloroethane in 1977 was about 2-20 million pounds (Gordon et al. 1991; HSDB 1995; IARC 1979; Kitchens et al. 1978; Santodonato et al. 1985; SRI 1977). Table 4-1 lists information on U.S. companies that reported the manufacture and processing of hexachloroethane in 1993 (TRI93 1995). The Toxics Release Inventory (TRI) data should be used with caution since only certain types of facilities are required to report. This is not an exhaustive list. HEXACHLOROETHANE 102 4. PRODUCTION, IMPORT, USE, AND DISPOSAL Table 4-1. Facilities That Manufacture or Process Hexachloroethane Range of maximum amounts on site Number of in thousands c State? facilities of pounds P Activities and uses CA 2 0-100 1,5,6,7, 11 IL 3 0-10000 2,3,4,8,9 IN 1 1-10 11 KS 1 100-1000 1.8 LA 5 1-100 1,3,5,6,7,11,13 Mi 1 10-100 7 MO 1 1-10 5 MS 1 10-100 12 NJ 2 10-100 2,4,9,10 OH 3 1-1000 2,389 1 TX 4 0-100 4.:8,86, 10,12 Source: TRI93 1995 2 Post office state abbreviations used b Data in TRI are maximum amounts on site at each facility ¢ Activities/Uses: 1. Produce 2. Import 3. For on-site use/processing 4. For sale/distribution 5. As a by-product 6. As an impurity 7. As a reactant 8. As a formulation component 9. As a product component 10. For repackaging only 11. As a chemical processing aid 12. As a manufacturing aid 13. Ancillary or other uses HEXACHLOROETHANE 103 4. PRODUCTION, IMPORT, USE, AND DISPOSAL 4.2 IMPORT/EXPORT Quantities of hexachloroethane imported into the United States increased from the 1970s to the 1980s. Imports were about 1.6 million pounds (730,000 kg) in 1976 (mainly from France and the United Kingdom), more than 2 million pounds in 1977, approximately 2.5 million pounds (1,124,000 kg) in 1985, and approximately 4.5 million pounds in 1986. In 1978, all hexachloroethane distributed commercially in the United States was imported by Rhodia, Inc., Monmouth, New Jersey. Current information on importers and import quantities was not located (ACGIH 1991; Gordon et al. 1991; HSDB 1995; IARC 1979; Kitchens et al. 1978; Santodonato et al. 1985). No data were located on export quantities, but exports are not expected, since hexachloroethane is not produced for commercial distribution. 4.3 USE Prior to 1979, 50% of the hexachloroethane distributed was used by the military for hexachloroethane smoke pots and grenades, 30-40% for the manufacture of degassing pellets to force air bubbles out of molten ore in aluminum foundries, and 10-20% as an anthelminthic to control sheep flukes. It has also been used as a moth repellent, a plasticizer for cellulose esters in place of camphor, a polymer additive, a component of fungicidal and insecticidal formulations, in the formulation of extreme pressure lubricants, and in the manufacture of fire extinguishing fluids. Currently, large amounts of hexachloroethane are still used by the military for hexachloroethane smoke and pyrotechnic devices. Hexachloroethane is probably not used any longer as an anthelminthic, since approval of the Food and Drug Administration (FDA) for this use of hexachloroethane was withdrawn in 1971 (ACGIH 1991; HSDB 1995; IARC 1979; Kitchens et al. 1978; Santodonato et al. 1985). Pine Bluff Arsenal in Arkansas was reported to be the major facility manufacturing smoke and pyrotechnic devices containing hexachloroethane for the military (Gordon et al. 1991). It was estimated that between 1966 and 1977 this facility used an average of 192,802 pounds of hexachloroethane annually (Kitchens et al. 1978). Data on quantities of hexachloroethane currently consumed for military and civilian uses were not located. HEXACHLOROETHANE 104 4. PRODUCTION, IMPORT, USE, AND DISPOSAL 4.4 DISPOSAL Hexachloroethane and waste containing hexachloroethane are classified as hazardous wastes by EPA. Generators of waste containing this contaminant must conform to EPA regulations for treatment, storage, and disposal (see Chapter 7). Rotary kiln or fluidized bed incineration methods are acceptable disposal methods for these wastes. Underground injection may also be used (HSDB 1995). According to the TRI, approximately 92,755 pounds of hexachloroethane were transferred to landfills and/or treatment/disposal facilities by industrial manufacturers or processors in 1993 (see Section 5.2) (TRI93 1995). No hexachloroethane was discharged to publicly owned treatment works (POTW), but 1,081 pounds were disposed of by underground injection. These data do not include disposal of hexachloroethane-containing wastes by the military. HEXACHLOROETHANE 105 5. POTENTIAL FOR HUMAN EXPOSURE 5.1 OVERVIEW Hexachloroethane is an industrial chemical which is not known to occur naturally. It is not produced for commercial distribution in the United States, but is imported for use in military smoke and pyrotechnic devices and as an intermediate in the organic chemicals industry. It is released to the environment from these uses, primarily to the atmosphere. Hexachloroethane is relatively persistent in the environment. It volatilizes readily from water to the atmosphere, with a half-life of less than one day in some waters. Hexachloroethane may also leach through soil to groundwater. Neither hydrolysis nor photolysis are expected to be important removal processes, but hexachloroethane may be reduced in aquatic systems in the presence of specific agents. Bioconcentration in fish has been reported, but biomagnification through the food chain is unlikely. Biodegradation may contribute to hexachloroethane removal from ambient waters, but there is conflicting evidence regarding the significance of this fate process for hexachloroethane. Hexachloroethane has been detected at low (ng/m®) levels in the atmosphere and occasionally in drinking water systems. It is rarely detected in surface waters or biota, and has not been reported in ambient soil, sediments, or commercial food products. Hexachloroethane has been identified in at least 45 of the 1,416 hazardous waste sites that have been proposed for inclusion on the EPA National Priorities List (NPL) (HazDat 1995). However, the number of sites evaluated for hexachloroethane is not known. The frequency of these sites within the United States can be seen in Figure 5-1. 5.2 RELEASES TO THE ENVIRONMENT Hexachloroethane is not known to occur naturally (IARC 1979). Most of the hexachloroethane entering environmental media is from releases during manufacture and use of the compound in smoke-producing and pyrotechnic devices and as an intermediate in the production of several other products (Gordon et al. FIGURE 5-1. FREQUENCY OF NPL SITES WITH HEXACHLOROETHANE CONTAMINATION * .. sletetet te, e343420el4, elelelatetetet, s30%02e%0%s el 020%434%4%4%0%, 23030320 %0t4, eteletetitatt, etetetetatatt, eleteletittat. eteleteletatt, sleet ete e telat, eet eteleteletat®atatstel, 00203033 % ete seers ee’, e203 4%4%0%e202, e202 edes%alatets steele, elele oe 2 ete’ eduledetelt, ota39%s%0%, etelaltatet, eteletet, eleleletet. eleleletets 2 e%2%4%%, o2wSet ely elelete’, elele’t, See. eteletetatet, ete. efeletatetat, etelatatat, etetetetatat, s2e%¢%0tn . ete . etelel fel tele . NPL sites [EE] 1 2 2 BEY 3 Bl i-5 *Derived from HAZDAT 1996 INVHLIOHOTHOVXIH JHNSOdX3 NYWNH HOH TVILN3LOd 'S 901t HEXACHLOROETHANE 107 5. POTENTIAL FOR HUMAN EXPOSURE 1991). Treatment and disposal of hexachloroethane-containing wastes also contributes to the environmental concentrations of this chemical. Recent data reported to the TRI indicate that environmental releases of hexachloroethane from manufacture and industrial processing total about 51,088 pounds (TRI93 1995). However, these data do not include releases from the manufacture and use of military smoke and pyrotechnic devices, since federal facilities are not required to report releases to the TRI. 5.2.1 Air The major sources of hexachloroethane releases to air are from its production and use in the organic chemical industry. As shown in Table 5-1, an estimated total of 49,716 pounds of hexachloroethane, amounting to about 97% of the total industrial environmental release, was discharged to the air from manufacturing and processing facilities in the United States in 1993 (TRI93 1995). The TRI data should be used with caution since only certain types of facilities are required to report. This is not an exhaustive list. Releases may also occur from the use of this chemical in smoke and pyrotechnic devices. Hexachloroethane content of the smoke devices is about 44.5-46% of the total solid material. The smoke device burns, producing smoke which is mainly zinc chloride, but contains some hexachloroethane. It was estimated that about 0.3-5% of the mass of the reagents in the device is released to air as hexachloroethane in the smoke, assuming a 70% burn efficiency (Katz et al. 1980; Novak et al. 1987). On this basis, it was estimated that during 1982-1984, a maximum of about 6,683 kg (14,700 pounds) of hexachloroethane was released to the atmosphere at Fort Irwin, California, a major military training facility (Novak et al. 1987). Hexachloroethane in smoke (aerosol) was measured in a wind tunnel at concentrations ranging from 0.64-1.26 mg/m’ (average 0.89 mg/m’) (Cataldo et al. 1989). Hexachloroethane may also be released to air during combustion and incineration of chlorinated wastes, from hazardous waste sites, and in small amounts during chlorination of sewage effluent prior to discharge and chlorination of raw water during drinking water treatment (Gordon et al. 1991; Howard 1989). Table 5-1. Releases to the Environment from Facilities That Manufacture or Process Hexachloroethane Range of reported amounts released in pounds per year ° Number of State” facilities Air ou enviroment Wo oo CA 2 0-5 0 0 0 0-5 0 0-1110 IL 3 0-7729 0 0 0 0-7729 0 0 IN 1 36005 0 0 0 36005 0 0 KS 1 10 0 0 1081 1091 0 645 LA 5 0-390 0- 0 0 0-390 0 0-760 Mi 1 2 0 0 0 2 0 41000 MO 1 500 0 0 0 500 0 0 MS 1 0 0 0 0 0 0 0 NJ 2 1-10 0 0 0 1-10 0 0 OH 3 0-738 0 0 0 0-738 0 0-46532 TX 4 0-110 0 0 0 0-400 0 0-2198 Source: TRI93 1995 a Data in TRI are maximum amounts released by each facility. b Post office state abbreviations used © The sum of all releases of the chemical to air, land, water, and underground injection wells by a given facility POTW = publicly owned treatment works INVHL3OHOTHOVYX3H FHNSOdX3 NYWNH HOH TVILN3LOd S 801 HEXACHLOROETHANE 109 5. POTENTIAL FOR HUMAN EXPOSURE 5.2.2 Water Releases of hexachloroethane to water may occur during production, processing, and disposal of the chemical. In the past, reported concentrations of hexachloroethane in manufacturing effluents and waste waters from industrial and POTW facilities ranged from 0.9 to 1,405.6 pg/L (Gordon et al. 1991). It is estimated that prior to 1979, about 117,000 gallons (443,000 liters) of waste water per day were released from the Pine Bluff Arsenal (Gordon et al. 1991). The average hexachloroethane concentration in the waste water was 168 mg/L, resulting in the release of about 165 pounds of hexachloroethane per day. Following installation of pollution abatement devices at the arsenal in 1979, hexachloroethane was not detected in several samples of waste water from the facility. Hexachloroethane was detectable in 2.0% of 1,253 effluent samples reported in the storage and retrieval (STORET) database maintained by EPA from 1980 to 1982 (Staples et al. 1985). The median concentration for all samples, including nondetects, was <10 pg/L. As shown in Table 5-1, an estimated total of 291 pounds of hexachloroethane, amounting to about 0.6% of the total industrial environmental release, was discharged to surface water from manufacturing and processing facilities in the United States in 1993 (TRI93 1995). An additional 1,081 pounds (2% of the total) was discharged to underground injection. The TRI data should be used with caution since only certain types of facilities are required to report. This is not an exhaustive list. 5.2.3 Sail Hexachloroethane may be released to soil by industrial sources and from hazardous waste sites at which this chemical has been detected. It may be also be released to soil from the use of hexachloroethane smoke and pyrotechnic devices via deposition of airborne particulates (see Section 5.3.1) (Cataldo et al. 1989) or ejection of partially reacted compounds from the canister by the force of combustion (Schaeffer et al. 1988). Average hexachloroethane concentrations in deposited residues from several smoke pots, using different burn configurations, ranged from 1,900 to 54,700 mg/kg (Schaeffer et al. 1988). The authors estimated that the soil load of hexachloroethane from a single upright canister (smoke pot) could reach 6,054 mg hexachloroethane per kg soil in a semicircular area with a 5 m radius downwind of the burn. HEXACHLOROETHANE 110 5. POTENTIAL FOR HUMAN EXPOSURE As shown in Table 5-1, no hexachloroethane was discharged to land from manufacturing and processing facilities in the United States in 1993 (TRI93 1995). The TRI data should be used with caution since only certain types of facilities are required to report. This is not an exhaustive list. 5.3 ENVIRONMENTAL FATE 5.3.1 Transport and Partitioning Hexachloroethane released to water or soil may volatilize into air or adsorb onto soil and sediments. Volatilization appears to be the major removal mechanism for hexachloroethane in surface waters (Howard 1989). The volatilization rate from aquatic systems depends on specific conditions, including adsorption to sediments, temperature, agitation, and air flow rate. Volatilization is expected to be rapid from turbulent shallow water, with a half-life of about 70 hours in a 2 m deep water body (Spanggord et al. 1985). A volatilization half-life of 15 hours for hexachloroethane in a model river 1 m deep, flowing 1 m/sec with a wind speed of 3 m/sec was calculated (Howard 1989). Measured half-lives of 40.7 and 45 minutes for hexachloroethane volatilization from dilute solutions at 25°C in a beaker 6.5 cm deep, stirred at 200 rpm, were reported (Dilling 1977; Dilling et al. 1975). Removal of 90% of the hexachloroethane required more than 120 minutes (Dilling et al. 1975). The relationship of these iaboratory data to volatilization rates from natural waters is not clear (Callahan et al. 1979). Atmospheric transport of hexachloroethane may occur, based on the stability of the compound in air (Class and Ballschmitter 1986; Singh et al. 1979). Hexachloroethane is expected to diffuse slowly into the stratosphere, with a half-life of about 30 years (Howard 1989). Deposition of hexachloroethane from air to water, plants, and soil has been reported (Cataldo et al. 1989). Based on calculated soil adsorption factors (log K_, of 2.24, 2.98, and 4.3), hexachloroethane is expected to have medium to low mobility in soil (Howard 1989). Thus, leaching to groundwater could occur. Results of studies with low organic carbon (0.02%) soil material indicate that sorption to aquifer materials retards hexachloroethane migration in groundwater (Curtis et al. 1986). In aquatic environments, moderate to slight adsorption to suspended solids and partitioning to sediments is likely (Howard 1989). Bioconcentration of hexachloroethane is expected to occur to a moderate degree. A measured bioconcentration factor (BCF) of 139 was reported in bluegills (EPA 1980a). After adjustment of the BCF HEXACHLOROETHANE 111 5. POTENTIAL FOR HUMAN EXPOSURE for lipid content, the weighted average BCF calculated for the edible portion of freshwater and estuarine aquatic organisms was 86.9. However, hexachloroethane is rapidly metabolized in bluegill, with an estimated half-life of <1 day (Howard 1989). The measured BCFs in rainbow trout were 510 and 1,200 at low (0.32 ng/L) and high (7.1 ng/L) exposure levels, respectively (Oliver and Niimi 1983). A BCF of 245 was calculated for hexachloroethane, based on the octanol water partition coefficient (K,,) and the molar solubility in octanol (Banerjee and Baughman 1991). Since hexachloroethane is rarely detected in ambient waters (see Section 5.4.2) and appears to be rapidly metabolized, significant bioaccumulation or biomagnification in the food chain is not expected. 5.3.2 Transformation and Degradation 5.3.2.1 Air Hexachloroethane is quite stable in air. It is not expected to react with hydroxyl radicals or ozone in the atmosphere or to photodegrade in the troposphere (Callahan et al. 1979; Howard 1989). Degradation by photolysis may occur in the stratosphere. 5.3.2.2 Water Hexachloroethane is also relatively resistant to degradation in the aquatic environment. No hydrolysis of hexachloroethane in water was observed after 11 days at 85°C at 3 pH levels (3, 7, and 11) (Ellington et al. 1987). However, hexachloroethane may be reduced in aquatic systems in the presence of sulfide and ferrous ions (Kriegman-King and Reinhard 1991). The transformation rate of hexachloroethane to tetrachloroethylene under simulated groundwater conditions at 50°C was evaluated without ferrous or sulfide ions, with minerals (biotite and vermiculite) providing ferrous ions, and with minerals and sulfide ions. Reported half-lives for hexachloroethane were 365 days for hexachloroethane alone, 57-190 days with minerals present, and 0.45-0.65 days in the presence of both minerals and sulfide. Photolysis of hexachloroethane in water has been reported, but degradation to carbon dioxide occurred at a temperature of 90-95°C (Knoevenagel and Himmelreich 1976). The relevance of these results to ambient conditions are uncertain. HEXACHLOROETHANE 112 5. POTENTIAL FOR HUMAN EXPOSURE Biodegradation may be an important removal process in ambient waters, but there is conflicting evidence regarding the significance of this fate process for hexachloroethane. In the presence of a mixed bacterial culture, hexachloroethane had no effect on the growth rate of the culture, was recovered quantitatively after incubation with the culture for 8 days, and hexachloroethane could not be used as a sole source of carbon after incubation for more than 6 weeks (Mrsny et al. 1978). The authors concluded that hexachloroethane was apparently not toxic to or metabolized by bacteria, and used hexachloroethane as an internal standard to monitor the bacterial degradation of crude oil. Results reported in another biodegradation screening study indicated that <30% degradation of hexachloroethane occurred after a 2-week incubation period in activated sludge under aerobic conditions (Howard 1989). However, other studies indicate that considerable biodegradation of hexachloroethane may occur. In a 7-day static- screening-flask test at 25°C under aerobic conditions, 100% loss of hexachloroethane was reported, with no loss attributable to volatilization (Tabak et al. 1981). Other studies reported significant losses (38% loss in sterile control) resulting from volatilization under aerobic conditions (Spanggord et al. 1985). Under anaerobic conditions, loss of 90% of hexachloroethane was reported from pond water in 18 days, while no loss from sterile pond water was observed (Spanggord et al. 1985). A half-life of about 40 days was reported for hexachloroethane in an unconfined sand aquifer (Criddle et al. 1986). Laboratory studies with wastewater microflora cultures and aquifer material provided evidence for microbial reduction of hexachloroethane to tetrachloroethylene under aerobic conditions in this aquifer system (Criddle et al. 1986). In anaerobic groundwater, hexachloroethane reduction to pentachloroethane and tetrachloroethylene was found to occur only when the water was not poisoned with mercury chloride (Roberts et al. 1994). Pentachloroethane reduction to tetrachloroethylene occurred at a similar rate in both poisoned and unpoisoned water. From these results, Roberts et al. (1994) suggested that the reduction of hexachloroethane to tetrachloroethylene occurred via pentachloroethane. The first step, the production of pentachloroethane, was microbially mediated, while the production of tetrachloroethylene from pentachloroethane was an abiotic process. 5.3.2.3 Sediment and Soil Hexachloroethane may biodegrade in soil, but abiotic degradation processes are not expected to be significant. Hexachloroethane is biotransformed in soil under both aerobic and anaerobic conditions, but proceeds more rapidly in anaerobic soils (Spanggord et al. 1985). Loss of 99% of hexachloroethane was HEXACHLOROETHANE 113 5. POTENTIAL FOR HUMAN EXPOSURE reported after 4 days of incubation anaerobically and after 4 weeks under aerobic conditions. Volatilization contributed to aerobic losses. 5.4 LEVELS MONITORED OR ESTIMATED IN THE ENVIRONMENT 5.41 Air Since hexachloroethane is quite stable in air (see Section 5.3.2.1), it may tend to accumulate in the atmosphere. Based on limited data, typical background concentrations in the northern hemisphere were reported to range from 5 to 7 ppt (48-68 ng/m’) (Singh et al. 1979). Data reported on the National Ambient Volatile Organic Compounds Database indicate that hexachloroethane was detected at an average concentration of 0.001 ppb (9.7 ng/m’) in ambient air in the United States, based on 69 measurements (Shah and Heyerdahl 1988). The detected concentrations were in remote and rural areas (average 3.2 ppt (31 ng/m?)), rather than in urban and industrial locations (Howard 1989; Shah and Heyerdahl 1988). Hexachloroethane was detected in the atmosphere in Portland, Oregon at concentrations ranging from 2.8 to 4.1 ng/m* (Ligocki et al. 1985) and in air over the Atlantic Ocean at an average concentration of 0.5 ppt (4.8 ng/m’) in the northern hemisphere and 0.34 ppt (3.3 ng/m) in the southern hemisphere (Class and Ballschmiter 1986). 5.4.2 Water Hexachloroethane is rarely detected in ambient water. Data reported in the STORET database indicate that the chemical was detectable in only 1 of 882 (0.1%) ambient water samples (Staples et al. 1985). The median concentration for all samples was <10 pg/L. Hexachloroethane was detected in Lake Ontario water, but not in Lake Erie (International Joint Commission 1983). The concentration of hexachloroethane in Lake Ontario was reported at 0.02 ng/L (Oliver and Niimi 1983). It was also identified in leachate from a hazardous waste site in Niagara Falls, New York (Hauser and Bromberg 1982). Hexachloroethane was not detected in 86 samples of urban runoff from 15 cities analyzed for the National Urban Runoff Program (Cole et al. 1984). Hexachloroethane has occasionally been reported in drinking water in the United States. Hexachloroethane was detected in drinking water from Cincinnati, Ohio and three water supplies in the New Orleans area at concentrations ranging from 0.03 to 4.3 pg/L (Keith et al. 1976); in the municipal HEXACHLOROETHANE 114 5. POTENTIAL FOR HUMAN EXPOSURE water supply in Evansville, Indiana (Kleopfer and Fairless 1972); and in 4 of 16 samples of Philadelphia drinking water (Suffet et al. 1980). It was also reported in 19 of 31 samples from private wells within 1 mile of a toxic waste dump in Hardeman County, Tennessee, at a median concentration of 0.26 pg/L (Clark et al. 1982). 5.43 Sediment and Soil Data regarding hexachloroethane concentrations in soil or sediments are sparse. Hexachloroethane was not detectable in any of 356 sediment analyses reported in the STORET database (Staples et al. 1985). The median detection limit was 500 pg/kg. 5.4.4 Other Environmental Media Hexachloroethane has not generally been reported in foods. Hexachloroethane was not detected in 116 fish samples reported in the STORET database (Staples et al. 1985), nor was it detected in 28 fish sampl:s from 14 Lake Michigan tributaries (Camanzo et al. 1987). However, hexachloroethane was detected in 10 of 10 Lake Ontario rainbow trout at an average concentration of 0.03 ng/g (Oliver and Niimi 1983). No information was located regarding hexachloroethane in other foods. 5.5 GENERAL POPULATION AND OCCUPATIONAL EXPOSURE Exposure of the general population to hexachloroethane is expected to be low. Analysis of blood from 13 individuals, using a method with a detection limit of 0.028 ppb, did not identify hexachloroethane in any sample (Ashley et al. 1992). The chemical has not been frequently detected in any environmental medium. Ambient air is the most likely source of hexachloroethane for exposed individuals in the general population (Howard 1989). Due to the stability of hexachloroethane (see Section 5.3.2.1), it may remain in the atmosphere for extended periods. Workers in industrial facilities manufacturing or using hexachloroethane as an intermediate in the manufacture of other products may be exposed to the chemical by inhalation or dermal absorption. In addition, military or civilian personnel working with smoke or pyrotechnic devices may be exposed. Based on information collected for the National Occupational Exposure Survey, the National Institute for HEXACHLOROETHANE 115 5. POTENTIAL FOR HUMAN EXPOSURE Occupational Safety and Health (NIOSH) estimates that 8,515 workers were potentially exposed to hexachloroethane (NOES 1991). 5.6 POPULATIONS WITH POTENTIALLY HIGH EXPOSURES Residents or workers near hazardous waste sites containing hexachloroethane wastes or military training areas using smoke or pyrotechnic devices containing hexachloroethane may be exposed to higher than ambient levels. 5.7 ADEQUACY OF THE DATABASE Section 104(i)(5) of CERCLA, as amended, directs the Administrator of ATSDR (in consultation with the Administrator of EPA and agencies and programs of the Public Health Service) to assess whether adequate information on the health effects of hexachloroethane is available. Where adequate information is not available, ATSDR, in conjunction with the NTP, is required to assure the initiation of a program of research designed to determine the health effects (and techniques for developing methods to determine such health effects) of hexachloroethane. The following categories of possible data needs have been identified by a joint team of scientists from ATSDR, NTP, and EPA. They are defined as substance-specific informational needs that if met would reduce the uncertainties of human health assessment. This definition should not be interpreted to mean that all data needs discussed in this section must be filled. In the future, the identified data needs will be evaluated and prioritized, and a substance-specific research agenda will be proposed. 5.7.1 Identification of Data Needs Physical and Chemical Properties. The physical and chemical properties of hexachloroethane are sufficiently well characterized to allow estimation of its environmental fate (see Table 3-2) (EPA 1991a; Spanggord et al. 1985; Verschueren 1983; Weast 1986). On this basis, it does not appear that further research in this area is required at this time. HEXACHLOROETHANE 116 5. POTENTIAL FOR HUMAN EXPOSURE Production, Import/Export, Use, Release, and Disposal. Hexachloroethane is not manufactured for commercial distribution in the United States (Gordon et al. 1991; IARC 1979; Santodonato et al. 1985). However, current production as a by-product and import information are not available. Current uses of this chemical and the amounts consumed by each use, including military uses, were not located. This information would be helpful in assessing potential exposure to workers and the general population. The amount of the chemical disposed of by industrial facilities was reported to EPA (TRI93 1995), but information on quantities of hexachloroethane-containing wastes disposed of by military facilities was not located. Rotary kiln or fluidized bed incineration are acceptable methods for disposal of waste containing hexachloroethane (HSDB 1995). According to the Emergency Planning and Community Right-to-Know Act of 1986, 42 U.S.C. Section 11023, industries are required to submit substance release and off-site transfer information to the EPA. The Toxics Release Inventory (TRI), which contains this information for 1993, became available in 1995. This database is updated yearly and should provide a list of industrial production facilities and emissions. Environmental Fate. The environmental fate of hexachloroethane has been characterized (Gordon et al. 1991; Howard 1989; Spanggord et al. 1985). The chemical is relatively unreactive and degrades slowly in environmental media. In groundwater the half-life of hexachloroethane may range from 365 days to less than a day when minerals and sulfide are present (Kriegman-King and Reinhard 1991). Because hexachloroethane appears to remain in the atmosphere for long periods (half-life not available) and may migrate to groundwater (Callahan et al. 1979; Curtis et al. 1986; Howard 1989), additional studies of adsorption and intermediate partitioning might be useful to assess the potential for emission and transport of this chemical from hazardous waste sites. Bioavailability from Environmental Media. No data are available on the absorption of hexachloroethane following inhalation or dermal contact. However, systemic toxicity (though minimal) was observed and suggests that some absorption can occur by these routes (Weeks et al. 1979). Data from animal studies that used gavage in oil for exposure to hexachloroethane indicate that the compound can also be absorbed following oral exposure (Fowler 1969b; Mitoma et al. 1985). No data were located regarding the absorption of hexachloroethane from air, water, soil, or plant material. Hexachloroethane exists in the air almost entirely as a vapor and there are no known processes that would impair its bioavailability from this medium. Since there is some adsorption of hexachloroethane to suspended solids and sediments in water, bioavailability from water may be limited (Howard 1989). On the other hand, HEXACHLOROETHANE 117 5. POTENTIAL FOR HUMAN EXPOSURE hexachloroethane is not expected to adsorb to soil significantly (Howard 1989). Additional studies would be useful to determine the extent of bioavailability of hexachloroethane from contaminated air and drinking water near hazardous waste sites. Food Chain Bioaccumulation. Hexachloroethane in water may bioconcentrate in aquatic organisms to a moderate degree (Howard 1989), with a BCF of 139 reported in bluegills (EPA 1980a). Due to its rapid metabolism (Howard 1989) and the low incidence of hexachloroethane in ambient waters (Staples et al. 1985), food chain bioaccumulation is unlikely. Additional research in this area does not appear to be necessary at this time. Exposure Levels in Environmental Media. Hexachloroethane has been detected in smoke generated from smoke-producing devices during military training exercises (Katz et al. 1980; Novak et al. 1987). In the Northern hemisphere and the United States, hexachloroethane has been detected in air at concentrations in the parts per trillion (Howard 1989; Ligocki et al. 1985; Shah and Heyerdahl 1988; Singh et al. 1979). In water, concentrations in the parts per billion are occasionally detected (Cole et al. 1984; International Joint Commission 1983; Staples et al. 1985). Hexachloroethane was not found in any of 356 sediment samples (Staples et al. 1985). Additional information regarding hexachloroethane in soil or sediments was not available. Since this chemical is not prevalent in the environment, monitoring of ambient environmental media does not appear to be required at this time. However, monitoring of workplace air, and environmental media at hazardous waste sites and military training areas at which hexachloroethane has been detected would help to determine potential sources of exposure. Reliable monitoring data for the levels of hexachloroethane in contaminated media at hazardous waste sites are needed so that the information obtained on levels of hexachloroethane in the environment can be used in combination with the known body burden of hexachloroethane to assess the potential risk of adverse health effects in populations living in the vicinity of hazardous waste sites. Exposure Levels in Humans. Hexachloroethane has not been detected in human tissues as a result of exposure to this chemical from environmental media. Biological monitoring data were not located for populations surrounding hazardous waste sites. Hexachloroethane has been detected in the plasma of workers at concentrations of 7.3 + 6 pg/L, despite the use of protective equipment including disposable overalls and compressed-air-fed visors or full-facepiece masks with filters (Selden et al. 1994). Because of HEXACHLOROETHANE 118 5. POTENTIAL FOR HUMAN EXPOSURE protective equipment, exposure concentrations could not be related to plasma levels of hexachloroethane. This information is necessary for assessing the need to conduct health studies on these populations. Exposure Registries. No exposure registries for hexachloroethane were located. This substance is not currently one of the compounds for which a subregistry has been established in the National Exposure Registry. The substance will be considered in the future when chemical selection is made for subregistries to be established. The information that is amassed in the National Exposure Registry facilitates the epidemiological research needed to assess adverse health outcomes that may be related to exposure to this substance. 5.7.2 On-going Studies No on-going studies regarding human exposure were located. HEXACHLOROETHANE 119 6. ANALYTICAL METHODS The purpose of this chapter is to describe the analytical methods that are available for detecting, and/or measuring, and/or monitoring hexachloroethane, its metabolites, and other biomarkers of exposure and effect to hexachloroethane. The intent is not to provide an exhaustive list of analytical methods. Rather, the intention is to identify well-established methods that are used as the standard methods of analysis. Many of the analytical methods used for environmental samples are the methods approved by federal agencies and organizations such as EPA and the National Institute for Occupational Safety and Health (NIOSH). Other methods presented in this chapter are those that are approved by groups such as the Association of Official Analytical Chemists (AOAC) and the American Public Health Association (APHA). Additionally, analytical methods are included that modify previously used methods to obtain lower detection limits, and/or to improve accuracy and precision. 6.1 BIOLOGICAL MATERIALS Analytical methods are available for measuring hexachloroethane in blood, urine, feces, liver, kidney, and adipose tissues, and breath (Ashley et al. 1992; Fowler 1969a; Nolan and Karbowski 1978; Pellizzari et al. 1985a, 1985b). Gas chromatography (GC) is the usual method for detecting and measuring hexachloroethane in biological materials (Pellizzari et al. 1985a, 1985b). The chromatograph separates complex mixtures of organics and allows individual compounds to be identified and quantified by a detector. An electron capture detector (ECD) is often used to identify hexachloroethane (Fowler 1969b; Nolan and Karbowski 1978). A mass spectrometer (MS) coupled to the GC column provides unequivocal identification. Blood samples for analysis of volatile organic compounds (VOCs) including hexachloroethane should be collected into containers from which VOC contamination has been reduced (Ashley et al. 1992). Potassium oxalate/sodium fluoride is the recommended anti-coagulant. Blood samples should be placed on ice or refrigerated shortly after collection, and Ashley et al. (1992) recommend that analysis for VOCs be completed within 14 days. Hexachloroethane can be detected in tissues at levels as low as 0.001 pg/g (Nolan and Karbowski 1978) and recoveries range from 50 to 130%. Prior to analysis, hexachloroethane must be separated from the HEXACHLOROETHANE 120 6. ANALYTICAL METHODS biological sample matrix and prepared for introduction into the analytical instrument. Separation may be effected by purging with an inert gas (helium), and trapping on an adsorbent cartridge (Tenax GC®), followed by thermal desorption directly to the GC column (Pellizzari et al. 1985a, 1985b). Alternatively, hexachloroethane may be extracted from the matrix with hexane (Fowler 1969b; Nolan and Karbowski 1978). Details of selected analytical methods for hexachloroethane in biological samples are summarized in Table 6-1. 6.2 ENVIRONMENTAL SAMPLES Determination of hexachloroethane in air, water, soil, wastes, and food is usually by GC analysis (APHA 1992; EPA 1982, 1990a, 1990b, 1990c; NIOSH 1994; Yurawecz and Puma 1986). Several representative methods for quantifying hexachloroethane in each of these media are summarized in Table 6-2. NIOSH (1994) has developed an approved method for analysis of hexachloroethane in air and EPA has developed approved methods for analysis of hexachloroethane in drinking water (EPA 1989, 1991c¢), water/wastewater (EPA 1982, 1990c), and soil/sediment/waste (EPA 1990a, 1990b) samples. The APHA (1992) method is equivalent to an EPA approved method. Separation of hexachloroethane from environmental samples is usually by extraction with an organic solvent such as methylene chloride or acetonitrile (EPA 1982, 1990a, 1990b, 1990c; Yurawecz and Puma 1986). A supercritical fluid extraction protocol has been developed for extraction of organics from soils and sediments (Lopez-Avila et al. 1991), which may be applicable to hexachloroethane. Air samples are drawn through a solid sorbent material and desorbed with carbon disulfide (NIOSH 1994). Cleanup procedures, with Florisil, for example, may be required for some environmental matrices (Yurawecz and Puma 1986). In addition, co-eluting compounds may be eliminated from extracts of drinking water by high performance liquid chromatography (HPLC) prior to GC/MS analysis, thus improving the quality of analytical results (Thruston 1978). The electron capture detector (ECD) is most frequently used to identify hexachloroethane. A flame ionization detector (FID) may also be used (NIOSH 1994). When unequivocal identification is required, an MS coupled to the GC column may be employed. TABLE 6-1. Analytical Methods for Determining Hexachloroethane in Biological Samples Sample detection Percent Sample matrix Preparation method Analytical method limit recovery Reference Blood Purge and trap on Tenax GC/MS =3 ng/mL? =80° Pellizzari et al. GC cartridge; desorb 1985a thermally Blood Purge and trap on Tenax GC/MS 0.028 ppb 93-41 Ashley et al. GC cartridge; desorb 1992 thermally Adipose tissue Macerate tissue in water; GC/MS =6 ng/g’ =50° Pellizzari et al. tap on Tenax GC 1985a cartridge; desorb thermally Breath Collect on Tenax GC Capillary column No data =70-130 Pellizzari et al. cartridge; dry over calcium GC/MS 1985b sulfate; desorb thermally Urine Extract with hexane; GLC/ECD No data >90 Fowler 1969b successively wash with water, sodium hydroxide, hydrochloric acid, and water Feces Macerate under warm GLC/ECD No data >90 Fowler 1969b hexane; successively wash with water, sodium hydroxide, hydrochloric acid, and water SAOHL3IN TVOILATVNY 9 3INVHLIOHOTHOVX3H Lect TABLE 6-1. Analytical Methods for Determining Hexachloroethane in Biological Samples (continued) Sample detection Percent Sample matrix Preparation method Analytical method limit recovery Reference Blood, liver, Extract with hexane GC/ECD 0.001 pgl/g No data Nolan and kidney, fat Karbowski 1978 *Typical or expected values for halocarbons by this method. Data were not reported for hexachloroethane. ECD = electron capture detector; GC = gas chromatography; GLC = gas liquid chromatography; MS = mass spectrometry SAOHLIW TVOILATVYNY “9 INVHLIOHOTHOVYXIH acl TABLE 6-2. Analytical Methods for Determining Hexachloroethane in Environmental Samples Sample detection Percent Sample matrix Preparation method Analytical method limit recovery Reference Air Collect on activated GC/FID 0.01 mg/sample 98 NIOSH 1994 coconut shell charcoal in glass tube; desorb with carbon disulfide Water/waste Extract with methylene GC/ECD 0.03 pg/L 99 EPA 1982 water chloride; exchange to hexane; Florisil cleanup, if required Waste water Extract continuously with Isotope dilution, 10 pg/L No data EPA 1990c methylene chloride under capillary column alkaline and then acidic GC/MS conditions Water/waste Extract with methylene Packed column 1.6 pg/L 40-113 APHA 1992 water chloride under alkaline GC/MS and then acidic conditions Water/soil/ Extract with methylene Capillary column 1.6 pg/L? 83-96 EPA 1990a wastes chloride; exchange to GC/ECD hexane; Florisil or GPC cleanup, if required Water/soil/ Extract with methylene Packed column 0.03 pg/L* =74 EPA 1990b wastes chloride; exchange to GC/ECD hexane; Florisil or GPC cleanup, if required SAOHL3W TVOILATYNY 9 INVH130HOTHOVX3H e€ect TABLE 6-2. Analytical Methods for Determining Hexachloroethane in Environmental Samples (continued) Sample detection Percent Sample matrix Preparation method Analytical method limit recovery Reference Food (fish, Extract with acetonitrile; GC/ECD No data >80 Yurawecz and milk, butter, cleanup with Florisil; elute Puma 1986 corn oil) with petroleum ether and ethyl ether/petroleum ether ‘Method detection limit (MDL) in reagent water. Estimated quantitation limits for other matrices are: 10 MDL in groundwater, 670-10,000 MDL in soil, and 100,000 MDL in nonaqueous wastes. ECD = electron capture detector; FID = flame ionization detector; GC = gas chromatography; GPC = gel permeation chromatography; MS = mass spectrometry INVHI3OHOTHOVYX3IH SAOHL3INW IVOILATYNY 9 vel HEXACHLOROETHANE 125 6. ANALYTICAL METHODS 6.3 ADEQUACY OF THE DATABASE Section 104(1)(5) of CERCLA, as amended, directs the Administrator of ATSDR (in consultation with the Administrator of EPA and agencies and programs of the Public Health Service) to assess whether adequate information on the health effects of hexachloroethane is available. Where adequate information is not available, ATSDR, in conjunction with the NTP, is required to assure the initiation of a program of research designed to determine the health effects (and techniques for developing methods to determine such health effects) of hexachloroethane. The following categories of possible data needs have been identified by a joint team of scientists from ATSDR, NTP, and EPA. They are defined as substance-specific informational needs that if met would reduce the uncertainties of human health assessment. This definition should not be interpreted to mean that all data needs discussed in this section must be filled. In the future, the identified data needs will be evaluated and prioritized, and a substance-specific research agenda will be proposed. 6.3.1 Identification of Data Needs Methods for Determining Biomarkers of Exposure and Effect The presence of hexachloroethane in exhaled air, blood, and tissues can be determined using GC/MS (Ashley et al. 1992; Pellizzari et al. 1985a, 1985b). Separation by GC with electron capture detection and liquid chromatography have also been used to identify hexachloroethane in blood, tissues, urine, and/or fecal matter (Fowler 1969b; Gorzinski et al. 1985; Jondorf et al. 1957; Mitoma et al. 1985; Nolan and Karbowski 1978). These methods are sufficiently sensitive and selective to measure low levels of hexachloroethane and levels that may result in adverse effects. Since the metabolites of hexachloroethane are themselves xenobiotic compounds or are the metabolites of other xenobiotics, the parent compound serves as the only true biomarker of exposure. Endogenous production of hexachloroethane following carbon tetrachloride exposure necessitates the need for an exposure history even when hexachloroethane is detected in body tissues or fluids (Fowler 1969a). Additional studies correlating levels of hexachloroethane in various biological media with environmental exposures would be useful. No data were located regarding methods that identify biomarkers of hexachloroethane's toxic effects. Although hexachloroethane-induced hepatic damage can cause increases in serum levels of liver enzymes, HEXACHLOROETHANE 126 6. ANALYTICAL METHODS these enzyme changes are not specific to hexachloroethane exposure (Fowler 1969b; Weeks et al. 1979). In male rats, exposure to hexachloroethane is associated with the presence of granular and cellular casts in the urine (NTP et al. 1989). These effects are related to the formation of hyaline droplets in the male rat kidney. The formation of hyaline droplets is unique in male rats and is not indicative of the toxic effect of hexachloroethane. Therefore, they are not useful as biomarkers of effect. There is a need to identify compound-specific biomarkers for the effects of hexachloroethane exposure at this time. Methods for Determining Parent Compounds and Degradation Products in Environmental Media. Analytical methods are available to detect and quantify hexachloroethane in air, water, soil, wastes, and food (APHA 1992; EPA 1982, 1990a, 1990b, 1990c; NIOSH 1994; Yurawecz and Puma 1986). Air is the medium of most concern for human exposure to this chemical. Exposure may also occur from water, especially in the vicinity of hazardous waste sites or industrial sources. The existing analytical methods can provide determinations for hexachloroethane at levels sufficiently low to meet regulatory requirements and evaluate health effects (EPA 1982, 1990a, 1990b, 1990c; NIOSH 1994). Methods are also available to measure degradation products of hexachloroethane in environmental samples, but these products (e.g., tetrachloroethylene) are released to the environment from many other sources and are therefore not useful determinants of the environmental impact of this chemical. 6.3.2 On-going Studies The Environmental Health Laboratory Sciences Division of the National Center for Environmental Health, Centers for Disease Control, is developing methods for the analysis of hexachloroethane and other volatile organic compounds in blood. These methods use purge and trap methodology, high resolution gas chromatography, and magnetic sector mass spectrometry which gives detection limits in the low parts per trillion (ppt) range. On-going studies to improve analytical methods for hexachloroethane and related compounds include the EPA "Master Analytical Scheme" being developed for organic compounds in water (Michael et al. 1988) and the research in supercritical fluid extraction (Lopez-Avila et al. 1991; Wieboldt et al. 1988). Research continues on improving extraction, concentration, and elution techniques, and detection devices (Eichelberger et al. 1983, 1990; Ho et al. 1993; Pankow and Rosen 1988; Valkenburg and Munslow HEXACHLOROETHANE 127 6. ANALYTICAL METHODS 1989). These improvements are designed to overcome problems with sample preparation and increase sensitivity and reliability of the analyses. HEXACHLOROETHANE 129 7. REGULATIONS AND ADVISORIES Because of its potential to cause adverse health effects in exposed people, numerous regulations, and advisories have been established for hexachloroethane by various international, national, and state agencies. Major regulations and advisories pertaining to hexachloroethane are summarized in Table 7-1. ATSDR has calculated an MRL of 6 ppm for acute inhalation exposure to hexachloroethane based on a NOAEL of 48 ppm from a study in pregnant rats. The critical effect was tremors, which occurred during an 11-day exposure period at a LOAEL of 260 ppm (Weeks et al. 1979). The intermediate inhalation MRL of 6 ppm was also calculated from a NOAEL of 48 ppm observed in a 6-week study in which tremors were observed in rats exposed intermittently at 260 ppm (Weeks et al. 1979). An MRL of 1 mg/kg/day has been calculated for acute oral exposure to hexachloroethane based on a NOAEL of 100 mg/kg/day from a study in male rabbits (Weeks et al. 1979). Hepatic necrosis and degeneration were observed in the treated animals at doses of 320 and 1,000 mg/kg/day. An intermediate-duration MRL of 0.01 mg/kg/day has been calculated for oral exposure to hexachloroethane in the diet based on a NOAEL of 1 mg/kg/day from a study in male and female rats (Gorzinski et al. 1985). Enlargement of the hepatocytes was seen in male rats at doses of 15 and 62 mg/kg/day. Relative liver weights were increased in males and females at the 62 mg/kg/day dose. EPA has derived a chronic oral RfD of 0.001 mg/kg/day for hexachloroethane (IRIS 1995). This value is based on a NOAEL of 1 mg/kg/day for atrophy and degeneration of the renal tubules in rats exposed for 16 weeks (Gorzinski et al. 1985). The NOAEL was divided by an uncertainty factor of 1,000 to account for interspecies extrapolation, human variability, and the use of a subchronic study. EPA places medium confidence in this RfD (IRIS 1995). HEXACHLOROETHANE 7. REGULATIONS AND ADVISORIES 130 TABLE 7-1. Regulations and Guidelines Applicable to Hexachloroethane carcinogen Agency Description Information Reference INTERNATIONAL IARC Carcinogenic classification Group 3* IARC 1987 NATIONAL Regulations: a. Air EPA OAQPS Hazardous Air Pollutant Yes Public Law 101- 549 Section 112 NESHAP for Source Categories: Yes EPA 1992 Organic HAPs from Synthetic Organic Chemical Manufacturing Industry (proposed) OSHA PEL TWA 1 ppm (10 mg/m®), skin OSHA 1993 (29 CFR 1910.1000) b. Water: EPA OWRS General permits under NPDES Yes 40 CFR 122 General Pretreatment Regulations for Yes 40 CFR 403 Existing and New Sources of Pollution Hazardous substance Yes 40 CFR 116 Reportable quantity 100 pounds 40 CFR 117.3 c. Other: EPA OERR Reportable quantity 100 pounds EPA 1989 (40 CFR 302.4) EPA OSW Hazardous Waste Constituent Yes EPA 1980b (Appendix VIII) (40 CFR 261) Groundwater Monitoring List Yes EPA 1987b (Appendix IX) (40 CFR 264) Land Disposal Restrictions Yes EPA 1990d, 1991b (40 CFR 268) Toxicity Characteristic Leaching 3 mg/L EPA 1995 Procedure Limit (40 CFR 261.24) Burning of Hazardous Waste 3x10? mg/kg EPA 1991b boilers and industrial furnaces-residue concentration limit EPA OTS Toxic Chemical Release Reporting Yes EPA 1988b Rule (40 CFR 372) Health and Safety Data Reporting Yes EPA 1988b Rule (40 CFR 716.120) Guidelines: a. Air ACGIH TLV TWA 1 ppm (9.7 mg/m’) ACGIH 1993 A2 - suspect human carcinogen NIOSH PEL TWA 1 ppm; NIOSH 1990 occupational HEXACHLOROETHANE 7. REGULATIONS AND ADVISORIES 131 TABLE 7-1. Regulations and Guidelines Applicable to Hexachloroethane Regulations and Guidelines: a. Air Connecticut Kansas Massachusetts Nevada North Dakota Oklahoma Texas Vermont Virginia b. Water: Kansas Minnesota Acceptable ambient conditions 8-hour annual 24-hour annual 8-hour 8-hour 24-hour 30-minute annual annual 24-hour Drinking water standards and guidelines 50 pg/m’ 25x10" pug/m’ 53x10" pg/m’ 2.5x10" pg/m’ 2.38 mg/m’ 9.7x10? pg/m’ 2.0x10% pg/m’ 97 pg/m’ 10 pg/m’ 25x10" pgm’ 1.6x10? pg/m’ 1.9 pg/L 0.7 ug/L (continued) Agency Description Information Reference NATIONAL (Cont.) b. Water: EPA ODW Health Advisories Gordon et al. 1991 1-day (child) 5 mg/L 10-day (child) 5 mg/L Longer term (child) 100 pg/L Longer term (adult) 450 pg/L Lifetime (adult) 1 pg/L EPA OWRS Ambient Water Quality Criteria EPA 1980a Ingesting water and organisms 1.9 pg/L® Ingesting organisms only 8.74 pg/L c. Other: EPA RfD (oral) 1x10” mg/kg/day IRIS 1995 Carcinogenic classification Group C° IRIS 1995 Cancer slope factor (q,") IRIS 1995 q,” (oral) 14x10 (mg/kg/day) q,” (inhalation) 1.4x10° (mg/kg/day) NTP May reasonably be anticipated to be a NTP 1994 carcinogen STATE NATICH 1995 FSTRAC 1990 *Group 3: Not classifiable as to human carcinogenicity *Based on a lifetime incremental cancer risk of 1x10 ‘Group C: Possible human carcinogen ACGIH = American Conference of Governmental Industrial Hygienists; EPA = Environmental Protection Agency; HAP = Hazardous Air Pollutant; IARC = International Agency for Research on Cancer; NESHAP = National Emission Standards for Hazardous Air Pollutants; NIOSH = National Institute for Occupational Safety and Health; NPDES = National Pollutant Discharge Elimination System; NTP = National Toxicology Program; OAQPS = Office of Air Quality Planning and Standards; ODW = Office of Drinking Water; OERR = Office of Emergency and Remedial Response; OSHA = Occupational Safety and Health Administration; OSW = Office of Solid Waste; OTS = Office of Toxic Substances; OWRS = Office of Water Regulations and Standards; PEL = Permissible Exposure Limit; RfD = Reference Dose; TLV = Threshold Limit Value; TWA = Time-Weighted Average HEXACHLOROETHANE 133 8. 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Sensitivity improvement in infrared detection for supercritical fluid chromatography. Anal Chem 60:2422-2427. *Yaws C, Yang HC, Pan X. 1991. Henry's law constants for 362 organic compounds in water. Chemical Engineering 179-185. Young JY, Smart DA, Allen JT, et al. 1989. Field exposure of chemical school students and cadre to fog oil and hexachloroethane (HC) smokes. Frederick, MD: U.S. Army Biomedical Research & Development Laboratory. AD-A225-008. *Yurawecz MP, Puma BJ. 1986. Gas chromatographic determination of electron capture sensitive volatile industrial chemical residues in foods, using AOAC pesticide multiresidue extraction and cleanup procedures. J Assoc Off Anal Chem 69:80-86. HEXACHLOROETHANE 147 9. GLOSSARY Acute Exposure -- Exposure to a chemical for a duration of 14 days or less, as specified in the Toxicological Profiles. Adsorption Coefficient (K,) -- The ratio of the amount of a chemical adsorbed per unit weight of organic carbon in the soil or sediment to the concentration of the chemical in solution at equilibrium. Adsorption Ratio (Kd) -- The amount of a chemical adsorbed by a sediment or soil (i.e., the solid phase) divided by the amount of chemical in the solution phase, which is in equilibrium with the solid phase, at a fixed solid/solution ratio. It is generally expressed in micrograms of chemical sorbed per gram of soil or sediment. Bioconcentration Factor (BCF) -- The quotient of the concentration of a chemical in aquatic organisms at a specific time or during a discrete time period of exposure divided by the concentration in the surrounding water at the same time or during the same period. Cancer Effect Level (CEL) -- The lowest dose of chemical in a study, or group of studies, that produces significant increases in the incidence of cancer (or tumors) between the exposed population and its appropriate control. Carcinogen -- A chemical capable of inducing cancer. Ceiling Value -- A concentration of a substance that should not be exceeded, even instantaneously. Chronic Exposure -- Exposure to a chemical for 365 days or more, as specified in the Toxicological Profiles. Developmental Toxicity -- The occurrence of adverse effects on the developing organism that may result from exposure to a chemical prior to conception (either parent), during prenatal development, or postnatally to the time of sexual maturation. Adverse developmental effects may be detected at any point in the life span of the organism. Embryotoxicity and Fetotoxicity -- Any toxic effect on the conceptus as a result of prenatal exposure to a chemical; the distinguishing feature between the two terms is the stage of development during which the insult occurred. The terms, as used here, include malformations and variations, altered growth, and in utero death. EPA Health Advisory -- An estimate of acceptable drinking water levels for a chemical substance based on health effects information. A health advisory is not a legally enforceable federal standard, but serves as technical guidance to assist federal, state, and local officials. Immediately Dangerous to Life or Health (IDLH) -- The maximum environmental concentration of a contaminant from which one could escape within 30 min without any escape-impairing symptoms or irreversible health effects. Intermediate Exposure -- Exposure to a chemical for a duration of 15-364 days, as specified in the Toxicological Profiles. HEXACHLOROETHANE 148 9. GLOSSARY Immunologic Toxicity -- The occurrence of adverse effects on the immune system that may result from exposure to environmental agents such as chemicals. In Vitro -- Isolated from the living organism and artificially maintained, as in a test tube. In Vivo -- Occurring within the living organism. Lethal Concentration, (LC, ,) -- The lowest concentration of a chemical in air which has been reported to have caused death in humans or animals. Lethal Concentrations, (LCj,) -- A calculated concentration of a chemical in air to which exposure for a specific length of time is expected to cause death in 50% of a defined experimental animal population. Lethal Dose; o, (LD) -- The lowest dose of a chemical introduced by a route other than inhalation that is expected to have caused death in humans or animals. Lethal Doses, (LD) -- The dose of a chemical which has been calculated to cause death in 50% of a defined experimental animal population. Lethal Time, (L Ts) -- A calculated period of time within which a specific concentration of a chemical is expected to cause death in 50% of a defined experimental animal population. Lowest-Observed-Adverse-Effect Level (LOAEL) -- The lowest dose of chemical in a study, or group of studies, that produces statistically or biologically significant increases in frequency or severity of adverse effects between the exposed population and its appropriate control. Malformations -- Permanent structural changes that may adversely affect survival, development, or function. Minimal Risk Level -- An estimate of daily human exposure to a dose of a chemical that is likely to be without an appreciable risk of adverse noncancerous effects over a specified duration of exposure. Mutagen -- A substance that causes mutations. A mutation is a change in the genetic material in a body cell. Mutations can lead to birth defects, miscarriages, or cancer. Neurotoxicity -- The occurrence of adverse effects on the nervous system following exposure to chemical. No-Observed-Adverse-Effect Level NOAEL) -- The dose of chemical at which there were no statistically or biologically significant increases in frequency or severity of adverse effects seen between the exposed population and its appropriate control. Effects may be produced at this dose, but they are not considered to be adverse. Octanol-Water Partition Coefficient (K,,) -- The equilibrium ratio of the concentrations of a chemical in n-octanol and water, in dilute solution. Permissible Exposure Limit (PEL) -- An allowable exposure level in workplace air averaged over an 8- hour shift. HEXACHLOROETHANE 149 9. GLOSSARY q,* -- The upper-bound estimate of the low-dose slope of the dose-response curve as determined by the multistage procedure. The q,* can be used to calculate an estimate of carcinogenic potency, the incremental excess cancer risk per unit of exposure (usually pg/L for water, mg/kg/day for food, and pg/m’ for air). Reference Dose (RfD) -- An estimate (with uncertainty spanning perhaps an order of magnitude) of the daily exposure of the human population to a potential hazard that is likely to be without risk of deleterious effects during a lifetime. The RfD is operationally derived from the NOAEL (from animal and human studies) by a consistent application of uncertainty factors that reflect various types of data used to estimate RfDs and an additional modifying factor, which is based on a professional judgment of the entire database on the chemical. The RfDs are not applicable to nonthreshold effects such as cancer. Reportable Quantity (RQ) -- The quantity of a hazardous substance that is considered reportable under CERCLA. Reportable quantities are (1) 1 pound or greater or (2) for selected substances, an amount established by regulation either under CERCLA or under Sect. 311 of the Clean Water Act. Quantities are measured over a 24-hour period. Reproductive Toxicity -- The occurrence of adverse effects on the reproductive system that may result from exposure to a chemical. The toxicity may be directed to the reproductive organs and/or the related endocrine system. The manifestation of such toxicity may be noted as alterations in sexual behavior, fertility, pregnancy outcomes, or modifications in other functions that are dependent on the integrity of this system. Short-Term Exposure Limit (STEL) -- The maximum concentration to which workers can be exposed for up to 15 min continually. No more than four excursions are allowed per day, and there must be at least 60 min between exposure periods. The daily TLV-TWA may not be exceeded. Target Organ Toxicity -- This term covers a broad range of adverse effects on target organs or physiological systems (e.g., renal, cardiovascular) extending from those arising through a single limited exposure to those assumed over a lifetime of exposure to a chemical. Teratogen -- A chemical that causes structural defects that affect the development of an organism. Threshold Limit Value (TLV) -- A concentration of a substance to which most workers can be exposed without adverse effect. The TLV may be expressed as a TWA, as a STEL, or as a CL. Time-Weighted Average (TWA) -- An allowable exposure concentration averaged over a normal 8-hour workday or 40-hour workweek. Toxic Dose (TDs) -- A calculated dose of a chemical, introduced by a route other than inhalation, which is expected to cause a specific toxic effect in 50% of a defined experimental animal population. Uncertainty Factor (UF) -- A factor used in operationally deriving the RfD from experimental data. UFs are intended to account for (1) the variation in sensitivity among the members of the human population, (2) the uncertainty in extrapolating animal data to the case of human, (3) the uncertainty in extrapolating from data obtained in a study that is of less than lifetime exposure, and (4) the uncertainty in using LOAEL data rather than NOAEL data. Usually each of these factors is set equal to 10. HEXACHLOROETHANE A-1 APPENDIX A ATSDR MINIMAL RISK LEVEL The Comprehensive Environmental Response, Compensation, and Liability Act (CERCLA) [42 U.S.C. 9601 et seq.], as amended by the Superfund Amendments and Reauthorization Act (SARA) [Pub. L. 99-499], requires that the Agency for Toxic Substances and Disease Registry (ATSDR) develop jointly with the U.S. Environmental Protection Agency (EPA), in order of priority, a list of hazardous substances most commonly found at facilities on the CERCLA National Priorities List (NPL); prepare toxicological profiles for each substance included on the priority list of hazardous substances; and assure the initiation of a research program to fill identified data needs associated with the substances. The toxicological profiles include an examination, summary, and interpretation of available toxicological information and epidemiologic evaluations of a hazardous substance. During the development of toxicological profiles, Minimal Risk Levels (MRLs) are derived when reliable and sufficient data exist to identify the target organ(s) of effect or the most sensitive health effect(s) for a specific duration for a given route of exposure. An MRL is an estimate of the daily human exposure to a hazardous substance that is likely to be without appreciable risk of adverse noncancer health effects over a specified duration of exposure. MRLs are based on noncancer health effects only and are not based on a consideration of cancer effects. These substance-specific estimates, which are intended to serve as screening levels, are used by ATSDR health assessors to identify contaminants and potential health effects that may be of concern at hazardous waste sites. It is important to note that MRLs are not intended to define clean-up or action levels. MRLs are derived for hazardous substances using the no-observed-adverse-effect level/uncertainty factor approach. They are below levels that might cause adverse health effects in the people most sensitive to such chemical-induced effects. MRLs are derived for acute (1-14 days), intermediate (15-364 days), and chronic (365 days and longer) durations and for the oral and inhalation routes of exposure. Currently, MRLs for the dermal route of exposure are not derived because ATSDR has not yet identified a method suitable for this route of exposure. MRLs are generally based on the most sensitive chemical-induced end point considered to be of relevance to humans. Serious health effects (such as irreparable damage to the liver or kidneys, or birth defects) are not used as a basis for establishing MRLs. Exposure to a level above the MRL does not mean that adverse health effects will occur. HEXACHLOROETHANE A-2 APPENDIX A MRLs are intended only to serve as a screening tool to help public health professionals decide where to look more closely. They may also be viewed as a mechanism to identify those hazardous waste sites that are not expected to cause adverse health effects. Most MRLs contain a degree of uncertainty because of the lack of precise toxicological information on the people who might be most sensitive (e.g., infants, elderly, nutritionally or immunologically compromised) to the effects of hazardous substances. ATSDR uses a conservative (i.e., protective) approach to address this uncertainty consistent with the public health principle of prevention. Although human data are preferred, MRLs often must be based on animal studies because relevant human studies are lacking. In the absence of evidence to the contrary, ATSDR assumes that humans are more sensitive to the effects of hazardous substance than animals and that certain persons may be particularly sensitive. Thus, the resulting MRL may be as much as a hundredfold below levels that have been shown to be nontoxic in laboratory animals. Proposed MRLs undergo a rigorous review process: Health Effects/MRL Workgroup reviews within the Division of Toxicology, expert panel peer reviews, and agencywide MRL Workgroup reviews, with participation from other federal agencies and comments from the public. They are subject to change as new information becomes available concomitant with updating the toxicological profiles. Thus, MRLs in the most recent toxicological profiles supersede previously published levels. For additional information regarding MRLs, please contact the Division of Toxicology, Agency for Toxic Substances and Disease Registry, 1600 Clifton Road, Mailstop E-29, Atlanta, Georgia 30333. HEXACHLOROETHANE A-3 APPENDIX A MINIMAL RISK LEVEL WORKSHEETS Chemical Name: Hexachloroethane CAS Number: 67-72-1 Date: September 1996 Profile Status: ~~ Draft 3 Post-public comments Route: [x] Inhalation [ ] Oral Duration: [x] Acute [] Intermediate [] Chronic Graph Key: 4 Species: Rat Minimal Risk Level: 6 [] mg/kg/day [x] ppm Reference: Weeks et al. 1979 Experimental design: Groups of 22 pregnant Sprague-Dawley rats were exposed to vapors of hexachloroethane (0, 15, 48, or 260 ppm) 6 hours/day on gestation days 6-16. Specific details of methods and results are not reported in this paper. Effects n in st n IT! ndin Hexachloroethane resulted in tremors at 260 ppm, with no neurological effects at 48 ppm. Transient mucopurulent nasal exudate in 85% of the animals and an unspecified decrease in maternal weight gain were noted in animals at 48 ppm. This effect was considered a result of an endemic mycoplasma infection and was not observed at 48 ppm in the 6-week study (Weeks et al. 1979). The 260-ppm concentration is a serious LOAEL for neurological effects and the 48-ppm concentration is a NOAEL. Dose and end point used for MRL derivation: [X] NOAEL []LOAEL 48 ppm Uncertainty Factors used in MRL derivation: [ 1 3 for use of a minimal LOAEL [x] 3 for extrapolation from animals to humans [x] 10 for human variability Was a conversion used from ppm in food or water to a mg/body weight dose? No. If so, explain: If an inhala ion Human Equivalent Concentration was calculated using default values from EPA (1988a). 48 ppm [(0.22 m*/day/0.204 kg) / (20 m?/day/70 kg)] = 181 ppm her itional studi r inent information which len his M HEXACHLOROETHANE APPENDIX A Other than the study by Weeks et al. (1979), there are no inhalation studies useful for estimating an acute inhalation MRL. HEXACHLOROETHANE A-5 APPENDIX A Chemical Name: Hexachloroethane CAS Number: 67-72-1 Date: September 1996 Profile Status: ~~ Draft 3 Post-public comments Route: [x] Inhalation [ ] Oral Duration: [] Acute [x] Intermediate [] Chronic Graph Key: 14 Species: Rat Minimal Risk Level: 6 [] mg/kg/day [x] ppm Reference: Weeks et al. 1979 Experimental design: Groups of 25 male and 25 female Sprague-Dawley rats were exposed to vapors of hexachloroethane (0, 15, 48 or 260 ppm) 6 hours/day, 5 days/week for 6 weeks. Half of the animals were sacrificed at the end of the exposure period while the remainder were sacrificed 12 weeks after the end of the study. Quantitative data are not reported in this paper. Effects noted in study an IT ndin One male and one female rat exposed at 260 ppm died. There was an increased incidence of mycoplasma infection at 260 ppm that the authors attributed to hexachloroethane-induced potentiation of an endemic infection. Histopathologic changes were not observed in the brain, lungs, heart, liver, kidneys, spleen, eyes, bone marrow, trachea, nasal turbinates, thymus, stomach, small intestines, large intestines, pancreas, adrenal glands, bladder, testes, skin, skeletal muscle, and bone. Body weights (quantitative data not given) were reduced, and eye irritation was noted at 260 ppm. The high concentration is a serious effect level associated with tremors and less serious effects, reduced resistance to infection, eye irritation, and reduced body weight. The 48-ppm concentration is a NOAEL. Dose and end point used for MRL derivation: [x] NOAEL []LOAEL 48 ppm Uncertainty Factors used in MRL derivation: [1 10 for use of a LOAEL [x] 3 for extrapolation from animals to humans [x] 10 for human variability Was a conversion used from ppm in food or water to a mg/body weight dose? No. If so, explain: If an inhalation study in animals, list the conversion factors used in determining human equivalent dose: Human Equivalent Concentration was calculated using default values from EPA (1988a). HEXACHLOROETHANE A-6 APPENDIX A Other additional studies or pertinent information which lend support to this MRL: Other than the study by Weeks et al. (1979) there are no inhalation studies useful for estimating an intermediate inhalation MRL. Studies in guinea pigs and dogs confirm that 260 ppm hexachloroethane is a serious effect concentration; 4/10 guinea pigs, and 1/4 dogs died at this concentration. These studies do not clearly identify a less serious LOAEL that does not have some serious effects. The 48-ppm concentration is a NOAEL for the most sensitive toxicity endpoint in all three species. HEXACHLOROETHANE A-7 APPENDIX A Chemical Name: Hexachloroethane CAS Number: 67-72-1 Date: September 1996 Profile Status: ~~ Draft 3 Post-public comments Route: [1 Inhalation [x] Oral Duration: [x] Acute [] Intermediate [ ] Chronic Graph Key: 8 Species: Rabbit Minimal Risk Level: 1 [x] mg/kg/day [] ppm Reference: Weeks et al. 1979 xperimental design: Groups of five male New Zealand rabbits were treated by gavage with hexachloroethane in methyl cellulose for 12 days at 0, 100, 320, or 1,000 mg/kg/day. Body weights were recorded daily, clinical signs were monitored, and serum chemistry parameters were evaluated (alanine aminotransferase, aspartate aminotransferase, blood urea nitrogen, alkaline phosphatase, bilirubin, total protein, potassium, and sodium). Necropsies were performed 4 days after the last dose and organs (lungs, liver, kidneys, spleen, testes) were weighed. Histopathological examinations of selected tissues and organs (eye, brain, lung, kidney, liver, spleen, heart, stomach, pancreas, small intestine, large intestine, skeletal muscle, bone, urinary bladder, testes) were also conducted. in n in Liver degeneration and necrosis occurred in a dose-related manner at 320 and 1,000 mg/kg/day. Effects were characterized as fatty degeneration, coagulative necrosis, hemorrhage, ballooning degeneration, eosinophilic change, and hemosiderin-laden macrophages and giant cells. Comparable effects were not seen in the 100-mg/kg/day dose group (lowest dose tested). Also, liver weights increased at the highest dose tested, however, quantitative data were not provided for evaluation. For the most part, serum clinical chemistry parameters were not significantly affected, except that levels of potassium and glucose were decreased significantly at dose levels of 320 mg/kg/day or greater. No quantitative data were provided for evaluation. Toxic tubular nephrosis of the convoluted tubules was seen at dose levels of 320 and 1,000 mg/kg/day; however, comparable effects were not observed at the lowest dose tested (100 mg/kg/day). Effects observed among treatment groups did not occur in a dose-dependent manner. Minimal tubular nephrocalcinosis occurred in a dose-related manner at dose levels of 320 mg/kg/day or greater. Also, kidney weights increased significantly (p<0.05) at the highest dose tested. Quantitative data were not provided for evaluation. No treatment-related gross or histopathological lesions of the urinary bladder were reported. Body weights were reduced significantly (p<0.05) at exposure levels of 320 and 1,000 mg/kg/day. Effects were seen within 7 days after compound exposure in the highest dose group and within 10 days at the intermediate dose. No changes in body weight were found at 100 mg/kg/day, the lowest dose tested. Quantitative data were not provided for evaluation. Dose and end point used for MRL derivation: [x] NOAEL []LOAEL 100 mg/kg/day for lack of liver effects HEXACHLOROETHANE A-8 APPENDIX A ncertainty Factor in L derivation: [] 10 for use of a LOAEL [x] 10 for extrapolation from animals to humans [x] 10 for human variability Was a conversion used from ppm in food or water to a mg/body weight dose? No. If so, explain: h ditional i inent information which lend support to this MRL: There are no other acute oral studies of hexachloroethane which support this MRL. However, intermediate- duration oral studies of hexachloroethane in rats described further in the worksheet for the intermediate- duration oral MRL provide support that the liver is a target following oral exposure to hexachloroethane. HEXACHLOROETHANE A-9 APPENDIX A Chemical Name: Hexachloroethane CAS Number: 67-72-1 Date: September 1996 Profile Status: ~~ Draft 3 Post-public comments Route: [] Inhalation [x] Oral Duration: [] Acute [x] Intermediate [ ] Chronic Graph Key: 18 Species: Rat Minimal Risk Level: 0.01 [x] mg/kg/day [] ppm Reference: Gorzinski et al. 1985 Experi 1 design: Groups of 10 male and 10 female Fischer-344 rats were fed hexachloroethane in the diet for 16 weeks at levels that provided doses of 0, 1, 15, or 62 mg/kg/day. Procedures were taken to minimize volatilization from food, and the doses are actual doses rather than target doses. Body weights were monitored weekly and food consumption biweekly. At 13 weeks, blood samples were collected and analyzed for red cell count, hemoglobin concentration, and leukocyte counts. Urine specimens (13-week) were analyzed for pH, glucose, protein, ketones, occult blood, and urobilinogen. Blood samples taken at 16 weeks were analyzed for serum urea nitrogen, creatine, glutamate-pyruvate transaminase, and alkaline phosphatase. After sacrifice, the weights of the brain, heart, liver, kidneys, and testes were determined. The tissues of the organs were preserved and examined histologically. Effects noted i n IT ndin Liver weights were increased in male rats at the highest dose and there was swelling of the hepatocytes in males at the highest two doses. Differences were significant for absolute and relative liver weights at the highest dose. Increased relative liver weights were seen in females at the highest dose. The kidneys in the two highest male dose groups displayed tubular atrophy, hypertrophy, and dilation. At the highest dose, kidney weights were increased by 10% and relative kidney weight by 5.5%. These changes in the kidneys were not seen in females except at the highest dose. There were no differences in the urinalysis results for the controls and exposed animals. Histopathologic changes in other organs were not observed. The 15-mg/kg/day dose is considered a minimal LOAEL for swelling of hepatocytes, and the 1-mg/kg/day dose is a NOAEL. D n in for MRL derivation: [x] NOAEL []LOAEL 1 mg/kg/day for lack of liver effects i i rivati [1 10 for use of a LOAEL [x] 10 for extrapolation from animals to humans [x] 10 for human variability HEXACHLOROETHANE A-10 APPENDIX A If an inhalation study in animals, list the conversion factors used in determining human equivalent dose: Other additional studies or pertinent information which lend support to this MRL: Increased liver weights and an increase in the number of gamma glutamyl transpeptidase positive foci (dimethylnitrosoamine was used as an initiator), were reported in rats treated by gavage with hexachloroethane in corn oil at 497 mg/kg/day 5 days/week for 7 weeks (Milman et al. 1988; Story et al. 1986). No other doses were used in this study. Centrilobular necrosis was observed in female Fischer-344 rats treated by gavage with hexachloroethane in corn oil 5 days/week for 13 weeks (NTP 1989). No liver effects were observed at 94 mg/kg/day, suggesting that the LOAEL identified in the Gorzinski et al. (1985) study may be conservative. No liver effects were observed in female rats treated by gavage with hexachloroethane in corn oil 5 days/week for 2 years (NTP 1989) providing further support that the 15-mg/kg/day LOAEL observed in the Gorzinski et al. (1985) study may be conservative. HEXACHLOROETHANE B-1 APPENDIX B USER'S GUIDE Chapter 1 Public Health Statement This chapter of the profile is a health effects summary written in non-technical language. Its intended audience is the general public especially people living in the vicinity of a hazardous waste site or chemical release. If the Public Health Statement were removed from the rest of the document, it would still communicate to the lay public essential information about the chemical. The major headings in the Public Health Statement are useful to find specific topics of concern. The topics are written in a question and answer format. The answer to each question includes a sentence that will direct the reader to chapters in the profile that will provide more information on the given topic. Chapter 2 Tables and Figures for Levels of Significant Exposure (LSE) Tables (2-1, 2-2, and 2-3) and figures (2-1 and 2-2) are used to summarize health effects and illustrate graphically levels of exposure associated with those effects. These levels cover health effects observed at increasing dose concentrations and durations, differences in response by species, minimal risk levels (MRLs) to humans for noncancer end points, and EPA's estimated range associated with an upper- bound individual lifetime cancer risk of 1 in 10,000 to 1 in 10,000,000. Use the LSE tables and figures for a quick review of the health effects and to locate data for a specific exposure scenario. The LSE tables and figures should always be used in conjunction with the text. All entries in these tables and figures represent studies that provide reliable, quantitative estimates of No-Observed-Adverse- Effect Levels (NOAELs), Lowest-Observed-Adverse-Effect Levels (LOAELSs), or Cancer Effect Levels (CELS). The legends presented below demonstrate the application of these tables and figures. Representative examples of LSE Table 2-1 and Figure 2-1 are shown. The numbers in the left column of the legends correspond to the numbers in the example table and figure. LEGEND See LSE Table 2-1 (1) Route of Exposure One of the first considerations when reviewing the toxicity of a substance using these tables and figures should be the relevant and appropriate route of exposure. When sufficient data exists, three LSE tables and two LSE figures are presented in the document. The three LSE tables present data on the three principal routes of exposure, i.e., inhalation, oral, and dermal (LSE Table 2-1, 2-2, and 2-3, respectively). LSE figures are limited to the inhalation (LSE Figure 2-1) and oral (LSE Figure 2-2) routes. Not all substances will have data on each route of exposure and will not therefore have all five of the tables and figures. (2) Exposure Period Three exposure periods - acute (less than 15 days), intermediate (15-364 days), and chronic (365 days or more) are presented within each relevant route of exposure. In this example, an inhalation study of intermediate exposure duration is reported. For quick reference to health effects HEXACHLOROETHANE B-2 3) “4 (5) (6) (7 ®) 9) (10) (11) APPENDIX B occurring from a known length of exposure, locate the applicable exposure period within the LSE table and figure. Health Effect The major categories of health effects included in LSE tables and figures are death, systemic, immunological, neurological, developmental, reproductive, and cancer. NOAELSs and LOAELSs can be reported in the tables and figures for all effects but cancer. Systemic effects are further defined in the "System" column of the LSE table (see key number 18). Key to Figure Each key number in the LSE table links study information to one or more data points using the same key number in the corresponding LSE figure. In this example, the study represented by key number 18 has been used to derive a NOAEL and a Less Serious LOAEL (also see the 2 "18r" data points in Figure 2-1). Species The test species, whether animal or human, are identified in this column. Section 2.5, "Relevance to Public Health," covers the relevance of animal data to human toxicity and Section 2.3, "Toxicokinetics," contains any available information on comparative toxicokinetics. Although NOAELs and LOAELS are species specific, the levels are extrapolated to equivalent human doses to derive an MRL. Exposure Frequency/Duration The duration of the study and the weekly and daily exposure regimen are provided in this column. This permits comparison of NOAELs and LOAELSs from different studies. In this case (key number 18), rats were exposed to 1,1,2,2-tetrachloroethane via inhalation for 6 hours per day, 5 days per week, for 3 weeks. For a more complete review of the dosing regimen refer to the appropriate sections of the text or the original reference paper, i.e., Nitschke et al. 1981. System This column further defines the systemic effects. These systems include: respiratory, cardiovascular, gastrointestinal, hematological, musculoskeletal, hepatic, renal, and dermal/ocular. "Other" refers to any systemic effect (e.g., a decrease in body weight) not covered in these systems. In the example of key number 18, 1 systemic effect (respiratory) was investigated. NOAEL A No-Observed-Adverse-Effect Level (NOAEL) is the highest exposure level at which no harmful effects were seen in the organ system studied. Key number 18 reports a NOAEL of 3 ppm for the respiratory system which was used to derive an intermediate exposure, inhalation MRL of 0.005 ppm (see footnote "b"). LOAEL A Lowest-Observed-Adverse-Effect Level (LOAEL) is the lowest dose used in the study that caused a harmful health effect. LOAELS have been classified into "Less Serious" and "Serious" effects. These distinctions help readers identify the levels of exposure at which adverse health effects first appear and the gradation of effects with increasing dose. A brief description of the specific endpoint used to quantify the adverse effect accompanies the LOAEL. The respiratory effect reported in key number 18 (hyperplasia) is a Less serious LOAEL of 10 ppm. MRLs are not derived from Serious LOAELS. Reference The complete reference citation is given in chapter 8 of the profile. CEL A Cancer Effect Level (CEL) is the lowest exposure level associated with the onset of carcinogenesis in experimental or epidemiologic studies. CELs are always considered serious effects. The LSE tables and figures do not contain NOAELSs for cancer, but the text may report doses not causing measurable cancer increases. HEXACHLOROETHANE B-3 (12) APPENDIX B Footnotes Explanations of abbreviations or reference notes for data in the LSE tables are found in the footnotes. Footnote "b" indicates the NOAEL of 3 ppm in key number 18 was used to derive an MRL of 0.005 ppm. LEGEND See Figure 2-1 LSE figures graphically illustrate the data presented in the corresponding LSE tables. Figures help the reader quickly compare health effects according to exposure concentrations for particular exposure periods. (13) (14) (15) (16) a7) (18) 19) Exposure Period The same exposure periods appear as in the LSE table. In this example, health effects observed within the intermediate and chronic exposure periods are illustrated. Health Effect These are the categories of health effects for which reliable quantitative data exists. The same health effects appear in the LSE table. Levels of Exposure concentrations or doses for each health effect in the LSE tables are graphically displayed in the LSE figures. Exposure concentration or dose is measured on the log scale "y" axis. Inhalation exposure is reported in mg/m? or ppm and oral exposure is reported in mg/kg/day. NOAEL In this example, 18r NOAEL is the critical endpoint for which an intermediate inhalation exposure MRL is based. As you can see from the LSE figure key, the open-circle symbol indicates to a NOAEL for the test species-rat. The key number 18 corresponds to the entry in the LSE table. The dashed descending arrow indicates the extrapolation from the exposure level of 3 ppm (see entry 18 in the Table) to the MRL of 0.005 ppm (see footnote "b" in the LSE table). CEL Key number 38r is 1 of 3 studies for which Cancer Effect Levels were derived. The diamond symbol refers to a Cancer Effect Level for the test species-mouse. The number 38 corresponds to the entry in the LSE table. Estimated Upper-Bound Human Cancer Risk Levels This is the range associated with the upper-bound for lifetime cancer risk of 1 in 10,000 to 1 in 10,000,000. These risk levels are derived from the EPA's Human Health Assessment Group's upper-bound estimates of the slope of the cancer dose response curve at low dose levels (q,*). Key to LSE Figure The Key explains the abbreviations and symbols used in the figure. TABLE 2-1. Levels of Significant Exposure to [Chemical x] — Inhalation INVHLIOHOTHOVX3IH Exposure LOAEL (effect) Key to frequency/ NOAEL - figure? Species duration System (ppm) Less serious (ppm) Reference INTERMEDIATE EXPOSURE Systemic ! l | l | | 18 Rat 13 wk Resp 3 ® 10 (hyperplasia) Nitschke et al. 5d/wk 1981 6hr/d > 0 nh CHRONIC EXPOSURE 2 x @ Cancer | 38 Rat 18 mo 20 (CEL, multiple Wong et al. 1982 5d/wk organs) 7hr/d 39 Rat 89-104 wk 10 (CEL, lung tumors, NTP 1982 5d/wk nasal tumors) 6hr/d 40 Mouse 79-103 wk 10 (CEL, lung tumors, NTP 1982 5d/wk hemangiosarcomas) 6hr/d # The number corresponds to entries in Figure 2-1. b by an uncertainty factor of 100 (10 for extrapolation from animal to humans, 10 for human variability). CEL = cancer effect level; d = days(s); hr = hour(s); LOAEL = lowest-observed-adverse-effect level; mo = month(s); NOAEL = no-observed- adverse-effect level, Resp = respiratory; wk = week(s) v-9 — > Figure 2-1. Levels of Significant Exposure to [Chemical X] - Inhalation Acute Intermediate (<14 days) (15-364 days) Systemic Systemic N N > yd 2 S—— © RY RR & > SS SX : Sel (ppm) ° x & XX EX < XR RN Q < X Q <& XN i < O 10000 — 1000 — 0 & 37m 0 100 - © @® o Oo O @® 30r 3ar & 17r d 2m ® Doom ~~ 3ir ad @ 35m Pd 16r 24g 15: @ 22g21r O 28m® 20r O 27r 40m * 18r 22m 34r r 10 |— 3 33r Q er 1 1 fee | 104 — ! . 0.1 | 105 Estimated <— v Upper Bound 0.01 — J Human Cancer Key 106 Risk Levels 0.001 |— r Rat @ LOAEL for serious effects (animals) I Minimal risk level for effects 107 1 m Mouse ( LOAEL for less serious effects (animals) | other than cancer 0.0001 — h Rabbit (QO NOAEL (animals) g Guinea Pig CEL - Cancer Effect Level The number next to each point 0.00001 |— k Monkey * corresponds to entries in the accompanying table. 0.000001 |— Co . * Doses represent the lowest dose tested per study that produced a tumorigenic response and do not imply the existence of a threshold for the cancer end point. 0.0000001 '— INVHLIOHOTHOVX3H a XION3ddVY S-8 HEXACHLOROETHANE B-6 APPENDIX B Chapter 2 (Section 2.5) Relevance to Public Health The Relevance to Public Health section provides a health effects summary based on evaluations of existing toxicologic, epidemiologic, and toxicokinetic information. This summary is designed to present interpretive, weight-of-evidence discussions for human health end points by addressing the following questions. 1. What effects are known to occur in humans? 2. What effects observed in animals are likely to be of concern to humans? 3. What exposure conditions are likely to be of concern to humans, especially around hazardous waste sites? The section covers end points in the same order they appear within the Discussion of Health Effects by Route of Exposure section, by route (inhalation, oral, dermal) and within route by effect. Human data are presented first, then animal data. Both are organized by duration (acute, intermediate, chronic). In vitro data and data from parenteral routes (intramuscular, intravenous, subcutaneous, etc.) are also considered in this section. If data are located in the scientific literature, a table of genotoxicity information is included. The carcinogenic potential of the profiled substance is qualitatively evaluated, when appropriate, using existing toxicokinetic, genotoxic, and carcinogenic data. ATSDR does not currently assess cancer potency or perform cancer risk assessments. Minimal risk levels (MRLs) for noncancer end points (if derived) and the end points from which they were derived are indicated and discussed. Limitations to existing scientific literature that prevent a satisfactory evaluation of the relevance to public health are identified in the Data Needs section. Interpretation of Minimal Risk Levels Where sufficient toxicologic information is available, we have derived minimal risk levels (MRLs) for inhalation and oral routes of entry at each duration of exposure (acute, intermediate, and chronic). These MRLs are not meant to support regulatory action; but to acquaint health professionals with exposure levels at which adverse health effects are not expected to occur in humans. They should help physicians and public health officials determine the safety of a community living near a chemical emission, given the concentration of a contaminant in air or the estimated daily dose in water. MRLs are based largely on toxicological studies in animals and on reports of human occupational exposure. MRL users should be familiar with the toxicologic information on which the number is based. Chapter 2.5, "Relevance to Public Health," contains basic information known about the substance. Other sections such as 2.7, "Interactions with Other Substances,” and 2.8, "Populations that are Unusually Susceptible" provide important supplemental information. MRL users should also understand the MRL derivation methodology. MRLs are derived using a modified version of the risk assessment methodology the Environmental Protection Agency (EPA) provides (Barnes and Dourson 1988) to determine reference doses for lifetime exposure (RfDs). HEXACHLOROETHANE B-7 APPENDIX B To derive an MRL, ATSDR generally selects the most sensitive endpoint which, in its best judgement, represents the most sensitive human health effect for a given exposure route and duration. ATSDR cannot make this judgement or derive an MRL unless information (quantitative or qualitative) is available for all potential systemic, neurological, and developmental effects. If this information and reliable quantitative data on the chosen endpoint are available, ATSDR derives an MRL using the most sensitive species (when information from multiple species is available) with the highest NOAEL that does not exceed any adverse effect levels. When a NOAEL is not available, a lowest-observed-adverse-effect level (LOAEL) can be used to derive an MRL, and an uncertainty factor (UF) of 10 must be employed. Additional uncertainty factors of 10 must be used both for human variability to protect sensitive subpopulations (people who are most susceptible to the health effects caused by the substance) and for interspecies variability (extrapolation from animals to humans). In deriving an MRL, these individual uncertainty factors are multiplied together. The product is then divided into the inhalation concentration or oral dosage selected from the study. Uncertainty factors used in developing a substance-specific MRL are provided in the footnotes of the LSE Tables. HEXACHLOROETHA NE C-1 ACGIH ADME AML atm ATSDR BCF BEI BSC C CDC CEL CERCLA CFR Ci CLP cm CML CNS d DHEW DHHS DOL ECG EEG EPA EKG F F, FAO FEMA FIFRA fpm ft FR g GC gen HPLC hr IDLH IARC ILO in Kd APPENDIX C ACRONYMS, ABBREVIATIONS, AND SYMBOLS American Conference of Governmental Industrial Hygienists Absorption, Distribution, Metabolism, and Excretion acute myeloid leukemia atmosphere Agency for Toxic Substances and Disease Registry bioconcentration factor Biological Exposure Index Board of Scientific Counselors Centigrade Centers for Disease Control Cancer Effect Level Comprehensive Environmental Response, Compensation, and Liability Act Code of Federal Regulations curie Contract Laboratory Program centimeter chronic myeloid leukemia central nervous system day Department of Health, Education, and Welfare Department of Health and Human Services Department of Labor electrocardiogram electroencephalogram Environmental Protection Agency see ECG Fahrenheit first filial generation Food and Agricultural Organization of the United Nations Federal Emergency Management Agency Federal Insecticide, Fungicide, and Rodenticide Act feet per minute foot Federal Register gram gas chromatography generation high-performance liquid chromatography hour Immediately Dangerous to Life and Health International Agency for Research on Cancer International Labor Organization inch adsorption ratio HEXACHLOROETHA NE APPENDIX C kg kilogram kkg metric ton K,. organic carbon partition coefficient K.. octanol-water partition coefficient L liter LC liquid chromatography 1L.C,, lethal concentration, low 1.C,, lethal concentration, 50% kill LD,, lethal dose, low LD, lethal dose, 50% kill LOAEL lowest-observed-adverse-effect level LSE Levels of Significant Exposure m meter MA trans,trans-muconic acid mCi millicurie mg milligram min minute mL milliliter mm millimeter mm Hg millimeters of mercury mmol millimole mo month mppcf millions of particles per cubic foot MRL Minimal Risk Level MS mass spectrometry NCE normochromatic erythrocytes NIEHS National Institute of Environmental Health Sciences NIOSH National Institute for Occupational Safety and Health NIOSHTIC NIOSH's Computerized Information Retrieval System ng nanogram nm nanometer NHANES National Health and Nutrition Examination Survey nmol nanomole NOAEL no-observed-adverse-effect level NOES National Occupational Exposure Survey NOHS National Occupational Hazard Survey NPL National Priorities List NRC National Research Council NTIS National Technical Information Service NTP National Toxicology Program OSHA Occupational Safety and Health Administration PEL permissible exposure limit PCE polychromatic erythrocytes pg picogram pmol picomole PHS Public Health Service PMR proportionate mortality ratio ppb parts per billion ppm parts per million C-2 HEXACHLOROETHA NE APPENDIX C ppt parts per trillion REL recommended exposure limit RfD Reference Dose RTECS Registry of Toxic Effects of Chemical Substances sec second SCE sister chromatid exchange SIC Standard Industrial Classification SMR standard mortality ratio STEL short term exposure limit STORET STORAGE and RETRIEVAL TLV threshold limit value TSCA Toxic Substances Control Act TRI Toxics Release Inventory TWA time-weighted average UMDNJ University of Medicine and Dentistry New Jersey U.S. United States UF uncertainty factor yr year WHO World Health Organization wk week > greater than > greater than or equal to = equal to < less than £ less than or equal to %o percent ao alpha B beta 0 delta Y gamma pm micrometer ug microgram C-3 #r U. 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