key: cord-0074417-udjia6pe authors: Sirianansopa, Kantisa; Rassameehirun, Chavisa; Chomtho, Sirinuch; Suteerojntrakool, Orapa; Kongkiattikul, Lalida title: Optimal Enteral Nutrition Support Preserved Muscle Mass in Critically Ill Children date: 2022-01-25 journal: J Nutr Metab DOI: 10.1155/2022/7004543 sha: 2eab461a69387cac3c8b34d2478bce078d9616dc doc_id: 74417 cord_uid: udjia6pe BACKGROUND: Inflammation and immobility are the most relevant mechanisms that alter protein synthesis and increase protein breakdown. Protein catabolism is associated with morbidity and mortality in critically ill children. OBJECTIVE: To demonstrate the effectiveness of the routinely used enteral nutrition support guideline in preventing muscle breakdown in critically ill children. METHODS: A prospective cohort study was conducted in the pediatric intensive care unit (PICU) of a tertiary care hospital. Critically ill children (aged 1 month to 15 years) admitted to the PICU were enrolled. All patients were assessed for nutritional status and nutritional requirement. Enteral nutrition support following the guideline was initiated within the first 24 hours if no contraindication. The calorie target was defined either by direct measurement from indirect calorimetry or estimated from Schofield equation with protein target at least 1.5 g/kg/day. Anthropometric assessments and body composition measurements by bioelectrical impedance analysis (BIA) were examined at baseline and on the seventh day of the PICU admission. RESULTS: Sixty-three patients were enrolled in the study. The most common age group was 1–5 years old (38.1%). The length of PICU stay was 9.1 (SD = 12.7) days. Respiratory problems were the major cause of PICU admission (50.8%). Mechanical ventilation was required in 55.6% of the patients with the average duration of 6.3 (SD = 12.4) days. Undernutrition was found in 36.5% of the patients. Enteral feeding was the major route of nutrition support (95.2%). After the first week of admission, muscle mass was significantly preserved (p < 0.01). All patients received the nutrition support at their target energy and protein goal within the first week. The enteral feeding-related complication was reported in 1.6% of the patients. CONCLUSION: Protein catabolism during critically ill period can be minimized by optimal nutrition support. Nutrition practice using the enteral nutrition support guideline was effective in helping critically ill children reach their target caloric and protein intake. e metabolic response induced by critical illness activates catabolic pathways and causes resistance to anabolic signals, which leads to extensive muscle wasting and loss of muscle function [1] . Catabolism of body protein due to starvation, immobility, stress, and inflammation has been described in pediatric patients with critical illness. Patients in pediatric intensive care unit (PICU) are at a high risk of developing low or depleted protein reserves. In addition, most of these patients already have chronic illness with associated malnutrition. ese conditions will increase their morbidity and mortality risks [2] . Protein depletion (15-25% of the total muscle mass) was reported during the first 10 days following admission to an intensive care unit [3] . Negative protein balance may result in loss of muscle mass which is associated with an increased length of hospital stay [4] . erefore, prevention of muscle breakdown in the first week of the critically ill period is a challenging nutrition goal in critical care. Various modalities of body composition measurement can be used in order to monitor the muscle mass of critically ill patients [5] . Bioelectrical impedance analysis (BIA), a method for estimating body composition, was used in this study. e advantages of BIA are that it is noninvasive, there is no radiation exposure, and it is a simple procedure that can be performed at bedside in the supine position. Body components were classified by the BIA technique, including conductive fluid, nonconductive fluid, and tissue components. Moreover, the accuracy of muscle mass measurements is not influenced by the hydration status of the patients [6] . Body cell mass (BCM) is a BIA parameter and represents the protein rich compartment of the human body which is affected by catabolic stages. Loss of BCM is associated with poor clinical outcome [7] . Another BIAderived parameter is phase angle. It was a correlation between the resistance and reactance vectors which indicated the cell membrane integrity and health fitness. PA has been studied as a prognostic marker in several health conditions including critically ill patients [8, 9] . Adequate nutrition support during the critically ill period is equally important to the recovery phase or rehabilitation period. Nutrition support focuses on reaching the energy goal with adequate micro-and macronutrients supplements. A lack of uniform bedside management tools could impact the nutrition outcome. Recently, the American Society for Parenteral and Enteral Nutrition (ASPEN) released a guideline for critically ill patients to achieve optimal nutrition support [10] . e previous nutrition practice guidelines in our institution were based on observational or retrospective data. To integrate with the update knowledge from the literature and the new ASPEN guideline, we developed an updated enteral nutrition support guideline for our own practice. A straightforward enteral nutrition support guideline consisted of five main concepts: (1) nutritional status and growth assessment, (2) nutritional requirement, (3) enteral nutrition advancement methods, (4) definition of gastrointestinal intolerance and stepwise approach management, and (5) bowel management strategies. is prospective study aimed to evaluate the effectiveness of our enteral nutrition support guideline. We hypothesized that (1) the protocol complying with the guideline would result in optimal nutrition support and consequently prevent muscle breakdown in critically ill children, and (2) optimizing nutrition therapy was a potential avenue of improving clinical outcomes in critically ill pediatric patients. is prospective cohort study was conducted at the pediatric intensive care unit, the King Chulalongkorn Memorial Hospital, a university-affiliated hospital. is 10-bed PICU was a mixed medical-surgical unit providing medical service at the tertiary care level. is study was approved by the Institutional Review Board, Faculty of Medicine, Chulalongkorn University, IRB No. 401/63. From September 2020 to February 2021, all critically ill children aged from 1 month to 15 years admitted to the PICU at least 48 hours were included in the study. Exclusion criteria were children with a contraindication to enteral feeding (e.g., postoperative gastrointestinal tract surgery) or unable to obtain body composition assessment by BIA (e.g., limb amputation). Sample size was calculated to detect a difference between the two means of dependent samples, with z � 1.96 or 95% confidence interval (CI) and bases on a standard deviation (SD) of 15 and the difference between the two groups of 6.3, reported by Hejazi et al. [11] . e calculated sample size of this study was 45. Baseline characteristics were recorded which included age, sex, admission diagnosis, length of PICU stay, length of mechanical ventilation, and the Pediatric Risk of Mortality PRISM III score. Nutrition status (determined by anthropometric assessments and body composition assessments) was assessed within 48 hours after PICU admission and on the 7 th day of admission. e pediatrics resident who was in charge of each patient was instructed to follow the enteral nutrition support guideline (Supplement 1). Primary outcome was changed from baseline in the quantity of muscle mass at the end of first week in the PICU. Secondary outcomes were impacts of nutrition practice on clinical outcomes. Anthropometric assessments were performed by welltrained pediatric residents. e measurements included weight, length or height, head circumference (only for children aged <36 months), mid-upper arm circumference (MUAC), and waist and hip circumference. For critically ill children who could not be weighed by a scale (e.g., mechanical ventilation or sedation), the weight was estimated by length/height measurement using the reference values from the World Health Organization (WHO) and nutrition status was classified by MUAC [12] . e anthropometric measurements categorized these patients in three main groups: normal nutrition status, protein energy malnutrition (weight for length/height < −3 Z-score), and obesity (weight for length/height > +3 Z-score) [13] . Body composition was measured by using BIA [7] (Bodystat ® : Quadscan 4000, U.K.). Four electrodes were connected to the right hand (wrist and middle fingers) and the right foot (ankle and above the knuckle of the toe) in the supine position. e BIA analysis took approximately 2 minutes to measure the whole-body compositions. e body compositions were examined twice at baseline and on the seventh day of admission in the morning. e BIA was performed by the same technician who is regularly using this instrument. BIA estimated the body components which included fat free mass (FFM), total body water (TBW), and body cell mass (BCM). All of the body components except 2 Journal of Nutrition and Metabolism fat is classified as FFM. BCM, a part of FFM, was a protein rich compartment without extracellular water (ECW) and associated with catabolic states. Phase angle (PA) was calculated from the values obtained from BIA and has been studied as a prognostic marker in several health conditions [10] . Energy expenditure was assessed by indirect calorimetry (IC) (CARESCAPE ™ R860, U.S.) in all mechanically ventilated patients [14] . If indirect calorimetry was not available or the patients were not intubated, an estimated resting energy expenditure (REE) was calculated from the Schofield equation without additional stress factors [15] . Our protocol did not calculate protein requirement but provided minimal protein intake at least 1.5 g/kg/day. All statistical analyses were performed using the R software, version 4.0.4 (Free Software Foundation, Inc., Boston, USA). Categorical variables were presented as frequency and percentage. Continuous variables were presented as mean with SD or median with interquartile range (IQR). e Wilcoxon signed-rank test was used to compare the mean difference (MD) of continuous data. e Spearmen's rank correlation test was used to assess relationships between the phase angle and mortality. A p value less than 0.05 indicated statistical significance. ere were 64 critically ill children admitted in the PICU during the study period, of which 63 were enrolled in this cohort study. One patient was excluded due to incomplete follow-up on body composition on the 7 th day from extensive severe skin infection. All of the patients compiled with the enteral nutrition support by the guideline. e patient characteristics are described in Table 1 . e reasons for admission were medical problems (79.3%), elective surgery (15.5%), and trauma/burn (3.2%). Medical problems included respiratory diseases (50.8%), cardiovascular diseases (14.3%), endocrine diseases (7.9%), and neurological diseases (6.3%). Energy expenditure was calculated by the Schofield equation, for REE (73% of the patients) and by indirect calorimetry (27%). Almost all of the patients (95.2%) received nutrition by enteral route. Muscle mass was measured by BIA and represented by BCM. e BCM after the first week of PICU admission was not decreased from the baseline (p < 0.01), as shown in Figure 1 . Mean difference and SD of BCM were 2.9 and 2.4 kg. e PA was significantly increased after the first week of PICU admission (MD 2.0, 95% CI 1.5-2.4). Furthermore, an association between the PA and the PRISM III score was observed. e lower PA value tended to correlate with higher PRISM III score (R � −0.1, 95% CI −0.34, 0.15). e nutritional and clinical outcomes are described in Table 2 . All of the patients achieved their target nutrition support, in both calories and protein, by the end of the first week. A majority of the patients (81%) received enteral feeding within 48 hours of PICU admission. Feeding e mean difference of muscle mass in the IC group was 2.9 (95% CI 2.1-3.7) and the Schofield equation group was 1.9 (95% CI 1.4-3.3), respectively ( Figure 2) . ere was no statistical difference between the groups (p � 0.01). Factors associated with feeding intolerance were delayed time (>48 hours after admission) to start enteral feeding (adjusted OR 1.4, 95% CI 0.18-10.95) and undernutritional status before admission (adjusted OR 1.1, 95% CI 0.16-7.02). Optimal nutrition therapy in the critically ill period is associated with lower odds of 60 d mortality [2] . Nutrition support in critically ill children may be challenging because acute illness can alter the patient's metabolism which causes difficulty in anticipating the individual calorie needs. Moreover, many factors, such as a lack of uniform feeding approach at the bedside, can interrupt nutrient delivery in PICUs. Many intensive care units developed their own nutrition support guideline following the ASPEN recommendation [10] . e guidelines aim to achieve the target calories and protein intake with an ultimate goal of improving both short-term and long-term clinical outcomes. Decreased muscle mass was reported during critical illness and was related to worse outcomes [11] . BIA is a method used for measuring body composition which included muscle mass [16] . is study measured BCM to represent the muscle mass in the patients who received enteral nutrition support following the guideline. e results demonstrated that the BCM was not significantly decreased after a week of PICU admission. We postulated that a nutrition support guideline could help critically ill children reach their target calories and protein intake. Our population from this study may be slightly different from usual due to COVID-19 pandemic as we did not have many severe critically ill patients. In contrast to previous studies, our patients achieved their caloric and protein target at the end of first week with a higher rate [17, 18] . Optimal nutrition management could help prevent muscle from breaking down. Minimal protein provided in our protocol was 1.5 g/kg/day; however, all patients in our study received at least 2 g/kg/day of protein intake at the end of first week. e important strategy of our guideline was aiming positive nitrogen balance which might be essential to offset the catabolic loss in critically ill children. Nevertheless, this study did not measure nitrogen balance which warrants further study. Weijs et al. [19] suggested at least 1.2 g/kg/day of protein intake for prevention of protein catabolism in the critically ill period. Our enteral nutrition support guideline was effective to minimize protein catabolism in the first week of critically ill period. Provision of adequate energy intake for critically ill children is associated with the calculation of REE. IC is the goal standard to estimate REE. If it is not feasible, the Schofield equation is an alternative method for calculating daily energy requirement [14] . e results of this study suggested that both IC and the Schofield equation provided the same primary outcome that the muscle mass was preserved during PICU admission. erefore, daily energy expenditure can be prescribed by using either method. Reaching the energy target was a potential goal; all patients in this study achieved their energy goal by the first week of PICU admission. Mehta et al. [20] revealed that an increase in energy intake from 33% to 66% of the prescription goal was associated with lower mortality (OR 0.27, 95% CI 0.11-0.67, p � 0.002). e considerable obstacles were feeding intolerance symptoms. A stepwise approach was recommended as a bedside management tool for physicians to overcome these nutrition barriers. ere were nonserious adverse events that occurred in our study period. e problem related to enteral feeding complication was observed only in 1.6% of the patients. Septic ileus occurred after encouraged bolus enteral feeding but was improved after conservative management. PA is another BIA-derived parameter besides the BCM. PA is associated with mortality outcomes and has stronger predictive power of mortality than the severity scoring systems commonly used in many intensive care units (OR 0.53, p < 0.01) [21] . Recently, Zamberlan et al. [22] showed a strong correlation of PA > 2.8 • with lower mortality rate in sepsis children (p < 0.01). is study found a negative correlation between the PA and PRISM III score (r � −0.1, 95% CI −0.34-0.15). A lower value of PA was associated with a higher severity score. Although this study was not designed to have enough power to detect this correlation, the trend of negative correlation was similar to another study [23] . PA could be used as an additional noninvasive indicator to predict prognosis in critically ill children. To our knowledge, this is the first study that demonstrates the efficacy of enteral nutrition support guideline by using BIA to monitor muscle mass in critically ill children. Limitations of this study included being conducted during the coronavirus pandemic period, and therefore, the number of our cases in PICU was limited, especially the elective surgery cases. e BIA was measured in the morning regardless of fasting status; however, this was measured by the same person throughout the study period. e schedule to follow up the patient after PICU discharge was canceled due to the pandemic. ere was no mortality in this study; therefore, we could not conclude this clinical outcome. ere was no patient who received only parenteral nutrition during the study period; thus, we could not illustrate the effectiveness of our nutrition guideline on this group. Further study is required to evaluate in other groups of critically ill children, especially one with extracorporeal organ support, and the long-term impact of nutrition management in critically ill children. Appropriate nutrition support during PICU admission plays a crucial role in the vital outcomes. Nutrition support guideline can be used for nutritional management in critically ill children which helps minimize protein catabolism. Nutrition practice using the enteral nutrition support guideline was effective in helping critically ill children reach their target caloric and protein intake. Data Availability e data that support the findings of this study are available from the first author upon request. e authors declare that they have no conflicts of interest. What factors influence protein synthesis and degradation in critical illness? 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Early high protein intake is associated with low mortality and energy overfeeding with high mortality in non-septic mechanically ventilated critically ill patients Nutritional practices and their relationship to clinical outcomes in critically ill children-An international multicenter cohort study Bioelectrical impedance analysis values as markers to predict severity in critically ill patients Bioelectrical impedance phase Angle and morbidity and mortality in critically ill children Phase angle and mortality: a systematic review Acknowledgments is research was supported by Ratchadapiseksompotch Fund (RA 63/089) and the authors wish to thank the English editing service, Research Affairs, Faculty of Medicine, Chulalongkorn University. Supplement 1: the enteral nutrition support protocol is used to guide enteral nutrition advancement methods and suggests management of gastrointestinal intolerance and bowel management strategies. (Supplementary Materials)