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达托霉素治疗影响万古霉素耐药粪肠球菌靶外种群的耐药性。

Daptomycin treatment impacts resistance in off-target populations of vancomycin-resistant Enterococcus faecium.

机构信息

Department of Internal Medicine, Division of Infectious Diseases, University of Michigan, Ann Arbor, Michigan, United States of America.

Center for Infectious Disease Dynamics and Department of Biology, Pennsylvania State University, University Park, Pennsylvania, United States of America.

出版信息

PLoS Biol. 2020 Dec 17;18(12):e3000987. doi: 10.1371/journal.pbio.3000987. eCollection 2020 Dec.

Abstract

The antimicrobial resistance crisis has persisted despite broad attempts at intervention. It has been proposed that an important driver of resistance is selection imposed on bacterial populations that are not the intended target of antimicrobial therapy. But to date, there has been limited quantitative measure of the mean and variance of resistance following antibiotic exposure. Here we focus on the important nosocomial pathogen Enterococcus faecium in a hospital system where resistance to daptomycin is evolving despite standard interventions. We hypothesized that the intravenous use of daptomycin generates off-target selection for resistance in transmissible gastrointestinal (carriage) populations of E. faecium. We performed a cohort study in which the daptomycin resistance of E. faecium isolated from rectal swabs from daptomycin-exposed patients was compared to a control group of patients exposed to linezolid, a drug with similar indications. In the daptomycin-exposed group, daptomycin resistance of E. faecium from the off-target population was on average 50% higher than resistance in the control group (n = 428 clones from 22 patients). There was also greater phenotypic diversity in daptomycin resistance within daptomycin-exposed patients. In patients where multiple samples over time were available, a wide variability in temporal dynamics were observed, from long-term maintenance of resistance to rapid return to sensitivity after daptomycin treatment stopped. Sequencing of isolates from a subset of patients supports the argument that selection occurs within patients. Our results demonstrate that off-target gastrointestinal populations rapidly respond to intravenous antibiotic exposure. Focusing on the off-target evolutionary dynamics may offer novel avenues to slow the spread of antibiotic resistance.

摘要

尽管已经广泛尝试进行干预,但抗菌药物耐药性危机仍在持续。有人提出,导致耐药性的一个重要驱动因素是对非抗菌药物治疗目标细菌群体的选择。但是到目前为止,对于抗生素暴露后耐药性的平均值和方差,还没有进行定量测量。在这里,我们关注的是医院系统中一种重要的医院获得性病原体粪肠球菌,尽管采取了标准干预措施,但该病原体对达托霉素的耐药性仍在不断演变。我们假设,达托霉素的静脉使用会在粪肠球菌可传播的胃肠道(携带)群体中产生针对耐药性的非靶向选择。我们进行了一项队列研究,比较了从接受达托霉素暴露的患者直肠拭子中分离出的粪肠球菌对达托霉素的耐药性,以及一组接受利奈唑胺暴露的患者,利奈唑胺是一种具有相似适应症的药物。在达托霉素暴露组中,来自非靶向人群的粪肠球菌对达托霉素的耐药性平均比对照组高 50%(n = 22 名患者的 428 个克隆)。在达托霉素暴露的患者中,达托霉素耐药性的表型多样性也更大。在那些随时间获得多个样本的患者中,观察到时间动态的广泛变异性,从长期维持耐药性到达托霉素治疗停止后迅速恢复敏感性。对部分患者分离株的测序支持了在患者体内发生选择的观点。我们的研究结果表明,非靶向胃肠道群体对静脉内抗生素暴露迅速作出反应。关注非靶向进化动态可能为减缓抗生素耐药性的传播提供新途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4478/7775125/55f378417cc2/pbio.3000987.g001.jpg

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