key: cord-0682844-er1e41y1
authors: de Carvalho, Fabrício Rodrigues Torres; Telles, João Paulo; Tuon, Felipe Francisco Bodan; Rabello Filho, Roberto; Caruso, Pedro; Correa, Thiago Domingos
title: Antimicrobial Stewardship Programs: A Review of Strategies to Avoid Polymyxins and Carbapenems Misuse in Low Middle-Income Countries
date: 2022-03-12
journal: Antibiotics (Basel)
DOI: 10.3390/antibiotics11030378
sha: 8f99b73e6bd6695b4dd57977b8c1f344ba4f3104
doc_id: 682844
cord_uid: er1e41y1

Antibiotics misuse and overuse are concerning issues worldwide, especially in low middle-income countries. These practices contribute to the increasing rates of antimicrobial resistance. One efficient strategy to avoid them is antimicrobial stewardship programs. In this review, we focus on the possible approaches to spare the prescription of polymyxins and carbapenems for the treatment of Acinetobacter baumannii, carbapenem-resistant Enterobacterales, and Pseudomonas aeruginosas infections. Additionally, we highlight how to implement cumulative antibiograms and biomarkers to a sooner de-escalation of antibiotics.

Antimicrobial resistance (AMR) has been discussed by the World Health Organization (WHO) since 2015 through the WHO Global Antimicrobial Resistance and Use Surveillance System (GLASS). In June 2021, WHO reported the fifth data from GLASS, accounting for more than a hundred countries [1] . The rates of bloodstream infections due to Escherichia coli resistant to third-generation cephalosporin and Staphylococcus aureus resistant to methicillin were higher in low middle-income countries compared with high-income countries (58% versus 17% and 33% versus 15%, respectively) [1] . Moreover, around 65% of all Acinetobacter spp. classified as a bloodstream infection were carbapenem-resistant [1] . In Europe, 30% of the Acinetobacter spp. and 12% of the Pseudomonas aeruginosa are resistant to multiple antimicrobial options (i.e., carbapenems, fluorquinolones, and aminoglycosides) (https://www.ecdc.europa.eu/sites/default/files/documents/surveillanceantimicrobial-resistance-Europe-2019.pdf; accessed on 1 May 2021). Additionally, it is expected that 10 million deaths each year will be due to drug-resistant bacteria in 2050 [2] .

Antimicrobial stewardship programs (ASP) play an important role in preventing the increase of AMR [3] . However, a meta-analysis demonstrated that there is heterogeinity in the included studies, and preventing the increase of AMR is better achieved when the infection prevention and control department develops activities along with the ASP team [4] . Additionally, there are different strategies of ASPs, such as prospective audit and feedback, preauthorization, or education programs. [5] . Nevertheless, it is recommended that all core elements such as education programs, along with antimicrobial restriction by prospective audit and feedback, are used together to improve outcomes (e.g., decreasing AMR and Clostridium difficille infection). It is important to highlight that, without hospital Antibiotics 2022, 11, 378 2 of 10 leadership commitment, ASP efforts may not be transformed into results. In different regions around the world, ASP has been demonstrated to be effective in decreasing AMR, Clostridioides difficille infection, and hospital costs [6] [7] [8] [9] .

There is evidence that "hit hard and hit fast" would be the best approach favoring the host instead of pathogen during the dynamics of an infection process, as previously thought by Paul Ehrlich in the beginning of the 20th century [10] . Nevertheless, it was never stated that the strength of the strategy would be related to its amplitude. Unfortunately, medical clinical practice commonly assumes that the harder you hit, the broader antimicrobial therapy you must prescribe. Antimicrobial de-escalation aims to attenuate the consequences of broad antimicrobial usage. However, as previously stated, this strategy should not be synonymous with safeguarding against inappropriate antibiotic prescription [11] . As diagnostic stewardship (e.g., a cumulative antibiogram analysis) favors a better understanding of the microbiological results, it allows a sooner de-escalation of the antibiotics, thus decreasing the antimicrobial selective pressure [12] .

The aim of this review is to highlight the alternatives to spare polymyxin and carbapenem usage to treat Acinetobacter baumannii, carbapenem-resistant Enterobacterales, and Pseudomonas aeruginosas infections. Moreover, we also describe how to implement cumulative antibiograms and biomarkers for a sooner de-escalation.

Polymyxin-based therapy remains as the gold standard for carbapenem-resistant Acinetobacter baumannii (CRAB) and extensively drug-resistant (XDR) Pseudomonas aeruginosa. However, these drugs have important disadvantages. Pharmacokinetics and pharmacodynamics data are scarce, susceptibility tests are based on broth microdilution, and side effects are common [13, 14] . Additionally, some regions of the globe have suffered polymyxin shortage during the COVID-19 pandemic, with a 400% increase in price (e.g., Brazil) [15] (https://oglobo.globo.com/saude/apos-vencerem-covid-19-pacientesmorrem-de-infeccao-hospitalar-por-falta-de-antibiotico-25123631; accessed on 1 November 2021) [16] . Therefore, alternative therapies are needed to avoid side effects and improve cost-effectiveness.

Considering the last data from Acinetobacter baumannii susceptibility, the results may differ between regions. For instance, data on multidrug-resistant (MDR) Acinetobacter baumannii from the United States of America (2014-2018) found that the MIC (minimum inhibitory concentration) 50-90 of levofloxacin, amikacin, cefepime, and meropenem were 4 mg/L, 8-32 mg/L, 16 mg/L, and 32 mg/L, respectively [17] . However, minocycline MIC 50-90 was 2-8 mg/L, while more than 70% of the isolates were minocycline-susceptible, according to the Clinical and Laboratorial Standards Institute [17] . Even in extensively drugresistant Acinetobacter baumannii strains (XDR), minocycline was the second-most active drug, with a 67% susceptibility, and polymyxin was the first, with 86% [17] . Between 2013 and 2016, the XDR Acinetobacter calcoacetius-Acinetobacter baumannii complex accounted for 86% of the isolates from Latin America, whereas the percentange was 40% in North America [18] . For these reasons, it is important to know the local susceptibility patterns for a better therapy choice.

Previous studies did not evaluate the outcomes of patients treated with polymyxins compared with alternative antibiotics. Nevertheless, cohort studies have demonstrated encouraging results of minocycline/doxycycline, sulfamethoxazole-trimethoprim (S-T), and sulbactam-based therapy [19] [20] [21] [22] . The tetracyclines (monotherapy or combined-based regimens) used depicted > 70% clinical success, including patients with ventilator-associated pneumonia (VAP) [19] [20] [21] .

Despite these results, caution should be taken, mainly to avoid tetracyclines monotherapy in patients with bloodstream infections, as these drugs present a large volume of distribution and low serum concentrations [23] . Sulfamethoxazole-trimethoprim is also an option when the susceptibility is known. A retrospective cohort found no differences in 30-day mortality between colistin versus S-T in monotherapy (38% versus 25%, respectively, p > 0.05) [23] . The major concerns of S-T use in critically ill patients are (i) the shortage of intravenous formulation on the market and (ii) the large volume of distribution, with a higher concentration in tissues [24] . Data on the total S-T serum concentrations showed that high-dose regimens (i.e., 2400 mg of sulfamethoxazole per day) can achieve serum concentrations higher than the MIC values [25] . However, free concentrations should be further investigated.

Sulbactam-based therapy may also be an option to spare polymyxins. The dosage regimen of sulbactam in critically ill patients should be at least 3 g q8h (1-h infusion) to achieve MICs as high as 8-16 mg/L [26] . A prospective cohort study compared sulbactam versus polymyxin in patients with VAP and found similar mortality rates between the regimens [27] . Unfortunately, MIC 50-90 of 8-16 mg/L for sulbactam in Acinetobacter calcoacetius-A. baumannii isolates were only found in North America, whereas MIC 50 > 16 mg/L were usually found worldwide [18, 28] .

There has been an increased incidence of carbapenem-resistant Enterobacterales worldwide, mainly due to Klebsiella pneumoniae [29] . More than 50% of CRE isolates carry the bla KPC gene, and 13% of carbapenem resistance is due to metallo-beta-lactamase [29] . Among CRE isolates, the MIC 50-90 of tigecycline, polymyxin, and amikacin were 0.5-2 mg/L, 0.25-8 mg/L, and 16-32 mg/L, respectively [30] . Thus, the major therapeutic option according to these results should be tigecycline. Almost 90% of these CRE isolates were from North America and Europe [30] . In Latin American, studies have demonstrated similar tigecycline MIC distributions in carbapenems producing Enterobacterales but a lower MIC 50 of amikacin, 4 mg/L [31] . Unfortunately, the major increase of CRE in the past years occurred in Latin America. This region has poor access to the new therapeutic options such as ceftazidime-avibactam and meropenem-vaborbactam. Therefore, a co-resistance to carbapenem and polymyxin is usual there [29, 32, 33 ].

Although tigecycline MIC distribution is relatively low, caution is needed regarding the choice of therapy. Tigecycline 50 mg q12h commonly does not achieve enough serum concentration to treat patients with severe infections, and a higher dosage regimen such as 100 mg q12h is needed [34] . In addition, a combination therapy with CRE is commonly used, and there is evidence of antagonism (in vivo and in vitro) between tigecycline and meropenem [35] .

Aminoglycosides remain as an important option to treat CRE. Nevertheless, monotherapy is still a concern, depending upon the site of infection. Considering its pharmacokinetics, the use of high doses is needed in critically ill patients to achieve suitable serum concentrations to treat CRE infections (e.g., amikacin MIC of 8 mg/L and gentamicin MIC of 2 mg/L) [36, 37] , while epithelial lining fluid may still present low concentrations [38] . However, the methods to evaluate pulmonary concentrations are not well-established [39] . Additionally, polymyxin pulmonary penetration is poor, and a combined therapy with meropenem did not demonstrate better outcomes [39, 40] . Therefore, aminoglycosides monotherapy to treat lung infections needs further investigation.

New therapeutic options for CRE are based on new beta-lactamase inhibitors. Therapies based on avibactam, relebactam, and vaborbactam are the first treatment options if these MDR pathogens are found [41] . Unfortunately, these options are usually not available in low middle-income countries. 

Third-generation cephalosporin-resistant bacteria have increased continually since the 1990 decade. During this period, Enterobacterales with third-generation cephalosporin resistance accounted for 10-15%, while, in 2013-2016, it increased up to 20-25% [29] . Some countries such as Belgium, France, Germany, and Ireland more than tripled their thirdgeneration cephalosporin resistance rates [29] . Additionally, in Latin America, countries such as Brazil, Argentina, Mexico, Chile, and Honduras also convereged on an important increase of ESBL among Enterobacteriales [42] .

These resistant patterns are caused by an increase in Extended-Spectrum Beta-Lactamases (ESBLs) such as CTX-Ms [43, 44] . Consequentially, carbapenem prescription has increased and, as a result, the bacteria's resistance to it. Therefore, a sparing carbapenem regimen therapy plays an important role in breaking the Gram-negative bacilli resistance pathway. However, alternative therapies such as quinolones, aminoglycosides, and group 1 carbapenem (i.e., ertapenem) have only been studied in retrospective cohorts.

For a long time, quinolones were used as a carbapenem-sparing option for infections caused by ESBL or AmpC isolates. However, the increase of quinolones resistance in ESBLpositive bacteria has put them aside, at least as an empirical option. In North America, quinolone susceptibility patterns from urinary isolates of ESBL-positive E. coli vary only between 7 and 26% (i.e., Ciprofloxacin and Levofloxacin) [45] . Data from Asia and Pacific countries have demonstrated a 20-30% quinolone susceptibility in ESBL-positive E. coli also from urinary tract infections [46] . Intra-abdominal infections may present higher quinolone patterns of susceptibility. As an example, in Asia and Pacific countries, ESBLpositive K. pneumoniae presented 57% susceptibility [47] . Therefore, despite the possible co-resistance of third-generation cephalosporins and quinolones, ASP should be aware of the quinolone local resistance rate and evaluate its de-escalation as soon as possible.

Beta-lactam/beta-lactamases inhibitors (BL/BLI) such as piperacillin-tazobactam were commonly used in infections caused by ESBL and Amp-C isolates. The MERINO trial, which included only bloodstream infections, compared meropenem with piperacillintazobactam and found a higher 30-day mortality in the piperacillin-tazobactam patient subgroup [48] . The results of the study have been questioned, as methodological problems have been noted, such as the drug infusion time, false-positive sensitivity to piperacillintazobactam, and mortality more frequent in patients with cancer [49] . Thus, BL/BLI is still open to discussion, and new trials are ongoing [44] . Despite that, BL/BLI, including amoxicillin-clavulanate, may be interesting options for urinary tract infections [50] . Caution is needed to treat severe infections due to the lack of amoxicillin-clavulanate pharmacokinetics and pharmacodynamics data [51] .

Besides the use of aminoglycosides for CRE infection, amikacin and gentamicin also have a central role in the treatment of ESBL-and AmpC-positive isolates. Studies have demonstrated a high susceptibility pattern around 90-95% of ESBL-positive bacteria [45, 47] . However, as stated previously, it is necessary to be careful to interpret the clinically treatable MICs of amikacin and gentamicin and to consider the severity of infection (e.g., higher dosage regimen in critically ill patients). Renal toxicity has been evaluated, and in studies using the propensity score matching in different populations, the results demonstrated that septic patients treated with meropenem or aminoglycosides presented the same proportition of acute kidney injury [52] .

Ertapenem may be an option to spare meropenem and imipenem. A recent metaanalysis concluded that ertapenem prescription does not increase carbapenem resistance either in Pseudomonas aeruginosas or in Enterobacterales [53] . The dosage of ertapenem of 1 g q24h is an option for earlier hospital discharge, presenting good cost-effectiveness [54] .

Thus, despite being a carbapenem, the antimicrobial stewardship program can use ertapenem to spare carbapenem group 2.

In recent years, the concept of cumulative antibiogram has been applied to the decisionmaking process for antibiotic selection before the final antimicrobial susceptibility testing results. To define the best choice of antibiotics, the historical susceptibility profile of the hospital or the community must be acknowledged. In case a pathogen is identified, an alternative that best fits the profile of the patient should be sought. For the construction of the cumulative antibiogram, some premises defined by the Clinical Laboratory Standards Institution (CLSI) have been suggested and are contained in the document CLSI M39-A2 [55] . An example of a cumulative antibiogram is detailed in Figure 1. evaluated, and in studies using the propensity score matching in different populations, the results demonstrated that septic patients treated with meropenem or aminoglycosides presented the same proportition of acute kidney injury [52] .

Ertapenem may be an option to spare meropenem and imipenem. A recent metaanalysis concluded that ertapenem prescription does not increase carbapenem resistance either in Pseudomonas aeruginosas or in Enterobacterales [53] . The dosage of ertapenem of 1 g q24h is an option for earlier hospital discharge, presenting good cost-effectiveness [54] . Thus, despite being a carbapenem, the antimicrobial stewardship program can use ertapenem to spare carbapenem group 2.

In recent years, the concept of cumulative antibiogram has been applied to the decision-making process for antibiotic selection before the final antimicrobial susceptibility testing results. To define the best choice of antibiotics, the historical susceptibility profile of the hospital or the community must be acknowledged. In case a pathogen is identified, an alternative that best fits the profile of the patient should be sought. For the construction of the cumulative antibiogram, some premises defined by the Clinical Laboratory Standards Institution (CLSI) have been suggested and are contained in the document CLSI M39-A2 [55] . An example of a cumulative antibiogram is detailed in Figure 1 . The microbiological tests will support medical judgments and the decision-making process. This allows for the most appropriate antibiotic use, especially in the current era of multidrug resistance.

In setting up the cumulative antibiogram of Gram-negative bacilli, it is necessary to find the best scheme for the main infection site (e.g., bacteremia, respiratory tract, and urinary tract). It is also important to remember that the combined therapy is guided to extend the spectrum, not for synergism. Ideally, during the cumulative antibiogram, quinolones and carbapenem should be avoided to decrease the selective pressure for multidrug-resistant bacteria. In this case, combinations with aminoglycosides can be an option [6] . A previous study that evaluated the use of quinolones and aminoglycosides by a cumulative antibiogram as a carbapenem-sparing strategy showed a reduction of carbapenem resistance after one year [6] . Different from expected, after one year of The microbiological tests will support medical judgments and the decision-making process. This allows for the most appropriate antibiotic use, especially in the current era of multidrug resistance.

In setting up the cumulative antibiogram of Gram-negative bacilli, it is necessary to find the best scheme for the main infection site (e.g., bacteremia, respiratory tract, and urinary tract). It is also important to remember that the combined therapy is guided to extend the spectrum, not for synergism. Ideally, during the cumulative antibiogram, quinolones and carbapenem should be avoided to decrease the selective pressure for multidrug-resistant bacteria. In this case, combinations with aminoglycosides can be an option [6] . A previous study that evaluated the use of quinolones and aminoglycosides by a cumulative antibiogram as a carbapenem-sparing strategy showed a reduction of carbapenem resistance after one year [6] . Different from expected, after one year of increased use of aminoglycosides, the susceptibility of this antimicrobial class increased, which is justified by a reduction in the carbapenem efflux system in some MDR microrganisms.

In spite of a useful, cumulative antibiogram, the laboratorial and ASP team needs constant communication and larger files (e.g., Excel) with all the culture and susceptibility tests results. Lastly, a cumulative antibiogram analysis must be done carefully in order to avoid misinterpretation between the different antimicrobial options tested in one bacteria species and not in another.

A distinction between viral and bacterial infections is challenging, particularly during the initial clinical presentation. As an example, in COVID-19, the hyperinflammatory phase of the late phase is difficult to differentiate from a secondary bacterial infection [56] . Therefore, many patients tend to mistakenly receive antibiotic therapy.

From a clinical perspective, biomarkers may help in the diagnosis and prognosis. The ideal biomarker should present fast kinetics, high sensitivity, and specificity. Regularly, the most used markers for the follow-up of patients with bacterial infections are the white blood cell count and the C-reactive protein (CPR). Additionally, procalcitonin (PCT) has been widely studied for this purpose [57, 58] .

CRP is one of many nonspecific acute-phase reactants that are elevated during an inflammatory process. Since the CRP response to an inflammatory process is nonspecific, many clinicians have not adopted its use as a predictive and prognostic test in intensive care medicine [59] . Furthermore, the role of CRP as a predictor of infection, instead of inflammation, has become even more controversial since the introduction of PCT as a test in this regard. Comparing CRP with other inflammatory markers (specially PCT) can be difficult because of their different kinetics. The overall evidence suggests that PCT has much faster kinetics, both in its onset and offset, and may also be more specific than the CRP in diagnosing some infections [58] [59] [60] . Since the CRP test is widely available and relatively cheaper than PCT, it is likely to be widely used in many institutions, including in low-income countries. Although CRP is more widely used, evidence suggests that PCT could be more useful regarding decisions of starting and discontinuing antibiotics and could help decrease antibiotic consumption and mortality in the ICU [58, 60, 61] .

In some previous studies, PCT has proven useful in the early detection of bacterial infections, lower respiratory tract infections being the most widely studied [58, 62] . It has been shown that PCT levels have greater sensitivity and specificity than CPR levels for detecting and following up patients with bacterial infections [58] . A possible explanation is that viral infections elevate the interferon-gamma (IFN-γ) serum levels, reducing the upregulation of PCT, which justifies the high specificity of PCT for distinguishing viral from bacterial infections [63, 64] .

A meta-analysis, including a total of 3244 patients from 30 high-quality studies, found that PCT presented a ROC curve of 0.85 (95% CI: 0.81-0.88) to distinguish sepsis from a systemic inflammatory response syndrome (SIRS) of noninfectious origins, an excellent result [65] . As in one of the previously cited studies [58] , in this meta-analysis, the majority of the included studies were done in the ICU, while 60% of patients were diagnosed with sepsis [65] . Nevertheless, in spite of these promising results, another meta-analysis in which the majority of patients were not diagnosed with sepsis nor needed ICU support, the ROC curve was lower, 0.73 (95% CI: 0.69-0.76) [63] . Therefore, there is a possible difference of the bacterial sepsis ROC curve between critically ill and noncritically ill patients, demonstrating that the clinical decision should not be based only on PCT levels.

Recently, an international guideline was published recommending the use of PCT levels in intensive care patients to estimate the bacterial infection probability [66] . The cut-off value that contemplates a lower probability of bacterial infection was set at <0.5, but serial measurements of PCT in 24-48 h can be necessary [66] . Furthermore, PCTbased antibiotic stewardship protocols should not be applied to patients with chronic infections, such as osteomyelitis, abscess, and endocarditis [66] . In addition, a more recent meta-analysis focusing on a PCT-guided antibiotic in septic patients with different sites of infection included 11 randomized trials with 4482 patients and demonstrated lower mortality with PCT-guided therapy [61] . Moreover, the PCT-guided patient group was associated with a shorter treatment duration of antibiotics [61] . These results reaffirm the safety and effectiveness of this biomarker use, leading to adequate diagnosis and treatment, the cornerstones of antibiotic stewardship.

There is still a lack of data regarding using biomarkers in ASP with the objective of decreasing the consumption of carbapenems and polymyxins. Nonetheless, the current evidence for starting and stopping antibiotics based on PCT values and patterns, in addition to medical history, physical exams, and culture results, could impact the prescription of these drugs. For instance, an observational study that evaluated the effectiveness of a guideline based on serum PCT values showed no difference in mortality compared with the standard care but demonstrated a substantial reduction on the prescription of carbapenems [67] .

Alternative antimicrobials to treat MDR Acinetobacter baumannii, Pseudomonas aeruginosas, and Enterobacterales are probably good options to spare carbapenems and polymyxins, mainly in regions with a lack of resources. However, larger clinical trials are still needed. Additionally, strategies based on cumulative antibiograms and biomarkers, such as PCT, may also optimize the reduction of antimicrobial consumption. 

World Health Organization. Global Antimicrobial Resistance and Use Surveillance System (GLASS) Report: 2021

New Report Calls for Urgent Action to Avert Antimicrobial Resistance Crisis

Meropenem antimicrobial stewardship program: Clinical, economic, and antibiotic resistance impact

Are antimicrobial stewardship programs effective strategies for preventing antibiotic resistance? A systematic review

Center for Disease Control and Prevention. Core Elements of Hospital Antibiotic Stewardship Programs

A broad-spectrum beta-lactam-sparing stewardship program in a middle-income country public hospital: Antibiotic use and expenditure outcomes and antimicrobial susceptibility profiles

Impact of a 4-year antimicrobial stewardship program implemented in a Greek tertiary hospital

The impact of antimicrobial stewardship program implementation at four tertiary private hospitals: Results of a five-years pre-post analysis

Trends in mathematical modeling of host-pathogen interactions

Antibiotics 2022

Antimicrobial de-escalation as part of antimicrobial stewardship in intensive care: No simple answers to simple questions-A viewpoint of experts

Diagnostic Stewardship-Leveraging the Laboratory to Improve Antimicrobial Use

International Consensus Guidelines for the Optimal Use of the Polymyxins: Endorsed by the American College of Clinical Pharmacy (ACCP)

Nephrotoxicity prevalence in patients treated with polymyxins: A systematic review with meta-analysis of observational studies

Trend analysis of carbapenem-resistant Gram-negative bacteria and antimicrobial consumption in the post-COVID-19 era: An extra challenge for healthcare institutions

Após Vencerem a COVID-19, Pacientes Morrem de Infecção Hospitalar por Falta de Antibiótico

Stenotrophomonas maltophilia, and Burkholderia cepacia Complex: Results from the SENTRY Antimicrobial Surveillance Program

Antimicrobial Susceptibility of Acinetobacter calcoaceticus-Acinetobacter baumannii Complex and Stenotrophomonas maltophilia Clinical Isolates: Results From the SENTRY Antimicrobial Surveillance Program (1997-2016)

Tetracyclines for multidrug-resistant Acinetobacter baumannii infections

Bad bugs need old drugs: A stewardship program's evaluation of minocycline for multidrug-resistant Acinetobacter baumannii infections

Tetracyclines for treating multidrug-resistant Acinetobacter baumannii ventilator-associated pneumonia

Trimethoprim-sulfamethoxazole vs. colistin or ampicillin-sulbactam for the treatment of carbapenem-resistant Acinetobacter baumannii: A retrospective matched cohort study

Pharmacokinetic and Pharmacodynamic Profiling of Minocycline for Injection following a Single Infusion in Critically Ill Adults in a Phase IV Open-Label Multicenter Study (ACUMIN)

Tissue penetration and antimicrobial activity of standard-and high-dose trimethoprim/sulfamethoxazole and linezolid in patients with diabetic foot infection

Serum concentration of co-trimoxazole during a high-dosage regimen

Population pharmacokinetics and Monte Carlo simulations of sulbactam to optimize dosage regimens in patients with ventilator-associated pneumonia caused by Acinetobacter baumannii

Efficacy and safety of high-dose ampicillin/sulbactam vs. colistin as monotherapy for the treatment of multidrug resistant Acinetobacter baumannii ventilator-associated pneumonia

Comparison of ampicillin-sulbactam and imipenem-cilastatin for the treatment of acinetobacter ventilator-associated pneumonia

Variations in the Occurrence of Resistance Phenotypes and Carbapenemase Genes Among Enterobacteriaceae Isolates in 20 Years of the SENTRY Antimicrobial Surveillance Program

In vitro activity of meropenem/vaborbactam and characterisation of carbapenem resistance mechanisms among carbapenem-resistant Enterobacteriaceae from the 2015 meropenem/vaborbactam surveillance programme

Antibiotics 2022

In vitro activity of ceftazidime/avibactam and comparators against Gram-negative bacterial isolates collected from Latin American centres between 2015 and 2017

Polymyxin B Resistance in Carbapenem-ResistantKlebsiella pneumoniae

Ceftazidime-Avibactam as Salvage Therapy for Infections Caused by Enterobacteriales Coresistant to Carbapenems and Polymyxins

Efficacy and safety of high-dose tigecycline for the treatment of infectious diseases: A meta-analysis

Antagonistic effect between tigecycline and meropenem: Successful management of KPC-producing Klebsiella pneumoniae infection

Aminoglycosides in the Intensive Care Unit: What Is New in Population PK Modeling? Antibiotics

Revisiting the loading dose of amikacin for patients with severe sepsis and septic shock

Evaluation of Epithelial Lining Fluid Concentration of Amikacin in Critically Ill Patients With Ventilator-Associated Pneumonia

Intrapulmonary pharmacokinetics of antibiotics used to treat nosocomial pneumonia caused by Gram-negative bacilli: A systematic review

Colistin plus meropenem for carbapenem-resistant Gram-negative infections: In vitro synergism is not associated with better clinical outcomes

Emerging Treatment Options for Multi-Drug-Resistant Bacterial Infections

Extended spectrum β-lactamase producers among nosocomial Enterobacteriaceae in Latin America

Global epidemiology of CTX-M β-lactamases: Temporal and geographical shifts in genotype

Extended-spectrum β-lactamases: An update on their characteristics, epidemiology and detection

Susceptibility patterns and ESBL rates of Escherichia coli from urinary tract infections in Canada and the United States

High Prevalence of Extended-Spectrum Beta-Lactamases in Escherichia coli Strains Collected From Strictly Defined Community-Acquired Urinary Tract Infections in Adults in China: A Multicenter Prospective Clinical Microbiological and Molecular Study

Antimicrobial susceptibility of Gram-negative ESKAPE pathogens isolated from hospitalized patients with intra-abdominal and urinary tract infections in Asia-Pacific countries: SMART 2013-2015

Meropenem Versus Piperacillin-Tazobactam for Definitive Treatment of Bloodstream Infections Caused by AmpC β-Lactamase-Producing Enterobacter spp., Citrobacter freundii, Morganella morganii, Providencia spp., or Serratia marcescens: A Pilot Multicenter Randomized Controlled Trial (MERINO-2). Open Forum

Effect of Piperacillin-Tazobactam vs Meropenem on 30-Day Mortality for Patients With E coli or Klebsiella pneumoniae Bloodstream Infection and Ceftriaxone Resistance: A Randomized Clinical Trial

Clinical effectiveness of oral antimicrobial therapy for acute pyelonephritis caused by extended-spectrum β-lactamase-producing Enterobacteriales

Orally Administered Amoxicillin/Clavulanate: Current Role in Outpatient Therapy

Antimicrobial therapy with aminoglycoside or meropenem in the intensive care unit for hospital associated infections and risk factors for acute kidney injury

Carbapenem stewardship with ertapenem and antimicrobial resistance-a scoping review

Efficacy and cost comparison of ertapenem as outpatient parenteral antimicrobial therapy in acute pyelonephritis due to extended-spectrum beta-lactamase-producing Enterobacteriaceae

Analysis and Presentation of Cumulative Antibiograms: A New Consensus Guideline from the Clinical and Laboratory Standards Institute

Bacterial and Fungal Coinfection in Individuals With Coronavirus: A Rapid Review To Support COVID-19 Antimicrobial Prescribing

The Geneva Sepsis Network. Diagnostic Value of Procalcitonin, Interleukin-6, and Interleukin-8 in Critically Ill Patients Admitted with Suspected Sepsis

Serum Procalcitonin and C-Reactive Protein Levels as Markers of Bacterial Infection: A Systematic Review and Meta-analysis

An Update on C-reactive Protein for Intensivists

Use of plasma C-reactive protein, procalcitonin, neutrophils, macrophage migration inhibitory factor, soluble urokinase-type plasminogen activator receptor, and soluble triggering receptor expressed on myeloid cells-1 in combination to diagnose infections: A prospective study

Effect of procalcitonin-guided antibiotic treatment on clinical outcomes in intensive care unit patients with infection and sepsis patients: A patient-level meta-analysis of randomized trials

Procalcitonin for diagnosis of infection and guide to antibiotic decisions: Past, present and future

Biomarkers of Infection: Are They Useful in the ICU?

Procalcitonin to Distinguish Viral From Bacterial Pneumonia: A Systematic Review and Meta-analysis

Procalcitonin as a diagnostic marker for sepsis: A systematic review and meta-analysis

Procalcitonin (PCT)-guided antibiotic stewardship: An international experts consensus on optimized clinical use

Evaluation of procalcitonin as a contribution to antimicrobial stewardship in SARS-CoV-2 infection: A retrospective cohort study

Data Availability Statement: Not applicable.

The authors declare no conflict of interest.

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