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The role of combination therapy in the treatment of severe infections caused by carbapenem resistant gram-negatives: a systematic review of clinical studies

机译:联合治疗在耐肠道耐素造成严重感染治疗严重感染的作用:临床研究的系统综述

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Effective treatment of sepsis due to carbapenem-resistant Gram-negative bacteria (CR-GNB) remains a challenge for clinicians worldwide. In recent years, the combination of antibiotics has become the preferred treatment strategy for CR-GNB infection. However, robust evidence to support this approach is lacking. This systematic review aimed at critically evaluating all available antibiotic options for CR-GNB sepsis with particular focus on combination. We systematically searched published literature from January 1945 until December 2018 for observational comparative and non-comparative studies and randomized trials examining any antibiotic option for CR-GNB. Studies were included if reporting microbiologically-confirmed infection caused by Acinetobacter baumannii, Enterobacteriaceae/Klebsiella spp., or Pseudomonas aeruginosa, reporting at least one of the study outcomes, and definitive antibiotic treatment. Carbapenem-resistance was defined as phenotypically-detected in vitro resistance to at least one of the following carbapenems: doripenem, ertapenem, imipenem, meropenem. Each antibiotic regimen was classified as “defined” when at least the molecular class(es) composing the regimen was detailed. Primary outcomes were 30-day and attributable mortality. Bayesian network meta-analysis (NMA) approach was selected for quantitative synthesis to explore feasibility of pooling data on antibiotic regimens. A total of 6306 records were retrieved and 134 studies including 11,546 patients were included: 54 studies were on Acinetobacter, 52 on Enterobacteriaceae/Klebsiella, 21 on mixed Gram-negative, and 7 on Pseudomonas. Nine (7%) were RCTs; 19 prospective cohorts (14%), 89 (66%) retrospective, and 17 (13%) case series. Forty-one studies (31%) were multicentric. Qualitative synthesis showed an heterogeneous and scattered reporting of key-clinical and microbiological variables across studies. Ninety-two distinct antibiotic regimens were identified with 47 of them (51%, 5863 patients) not reporting any details on numbers, type, dosage and in vitro activity of the included antibiotic molecules. The NMAs could not be performed for any of the selected outcome given the presence of too many disconnected components. The existing evidence is insufficient to allowing for the formulation of any evidence-based therapeutic recommendation for CR-GNB sepsis. Future studies must provide a standardized definition of antibiotic regimen to drive recommendations for using combination of antibiotics that can be reliably applied to clinical practice.
机译:由于CarbapeNem抗性革兰氏阴性细菌(Cr-GNB)为脓毒症的有效治疗仍然是全世界临床医生的挑战。近年来,抗生素的组合已成为Cr-GNB感染的优选治疗策略。但是,缺乏支持这种方法的强大证据。这种系统审查旨在重视CR-GNB败血症的所有可用抗生素选择,特别关注组合。从1945年1月到2018年12月,我们系统地搜索了发布的文学,用于观察到的比较和非比较研究以及检查CR-GNB的任何抗生素选项的随机试验。如果报告由肺杆菌,肠杆菌菌,肠杆菌痤疮/ Klebsiella SPP引起的微生物诊断的感染,或假单胞菌铜绿假单胞菌,则包括研究。 Carbapenem抗性被定义为对以下至少一种的碳癌蛋白的体外抗性的表型抗性:Doripenem,ErtapeNem,Imipenem,Meropenem。每种抗生素方案被归类为“定义”,当组成的分子类别进行详细说明。主要成果为30天,可惜的死亡率。选择贝叶斯网络荟萃分析(NMA)方法进行定量合成,以探讨粘合数据的可行性抗生素方案。还检索了6306条记录,包括134项研究,包括11,546名患者:54项研究是在肠杆菌菌/克雷布氏菌的52项上,混合革兰氏阴性阴性和7次上的7例。九(7%)是RCT; 19次预期队列(14%),89(66%)回顾性,17(13%)案例系列。四十一项研究(31%)是多中心的。定性合成显示跨研究的关键临床和微生物变量的异质和分散报告。用其中47例鉴定了九十二种不同的抗生素方案(51%,5863名患者)未报告包含抗生素分子的数量,类型,剂量和体外活性的任何细节。鉴于存在太多断开组件的存在,无法对任何选定的结果进行NMA。现有证据不足以允许制定任何用于Cr-GNB败血症的基于证据的治疗建议。未来的研究必须提供抗生素方案的标准化定义,以推动使用可以可靠地应用于临床实践的抗生素组合的建议。

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