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大肠杆菌对抗生素耐药适应性代价的适应

Adaptation to the fitness costs of antibiotic resistance in Escherichia coli.

作者信息

Schrag S J, Perrot V, Levin B R

机构信息

Department of Biology, Emory University, Atlanta, GA 30322, USA.

出版信息

Proc Biol Sci. 1997 Sep 22;264(1386):1287-91. doi: 10.1098/rspb.1997.0178.

Abstract

Policies aimed at alleviating the growing problem of drug-resistant pathogens by restricting antimicrobial usage implicitly assume that resistance reduces the Darwinian fitness of pathogens in the absence of drugs. While fitness costs have been demonstrated for bacteria and viruses resistant to some chemotherapeutic agents, these costs are anticipated to decline during subsequent evolution. This has recently been observed in pathogens as diverse as HIV and Escherichia coli. Here we present evidence that these gentic adaptations to the costs of resistance can virtually preclude resistant lineages from reverting to sensitivity. We show that second site mutations which compensate for the substantial (14 and 18% per generation) fitness costs of streptomycin resistant (rpsL) mutations in E. coli create a genetic background in which streptomycin sensitive, rpsL+ alleles have a 4-30% per generation selective disadvantage relative to adapted, resistant strains. We also present evidence that similar compensatory mutations have been fixed in long-term streptomycin-resistant laboratory strains of E. coli and may account for the persistence of rpsL streptomycin resistance in populations maintained for more than 10,000 generations in the absence of the antibiotic. We discuss the public health implications of these and other experimental results that question whether the more prudent use of antimicrobial chemotherapy will lead to declines in the incidence of drug-resistant pathogenic microbes.

摘要

旨在通过限制抗菌药物使用来缓解耐药病原体这一日益严重问题的政策,隐含地假定在没有药物的情况下,耐药性会降低病原体的达尔文适应性。虽然已经证明对某些化疗药物耐药的细菌和病毒存在适应性代价,但预计这些代价在后续进化过程中会下降。最近在诸如艾滋病毒和大肠杆菌等多种病原体中都观察到了这一点。在此,我们提供证据表明,这些针对耐药代价的遗传适应实际上可能会阻止耐药谱系恢复为敏感状态。我们表明,补偿大肠杆菌中链霉素抗性(rpsL)突变所带来的巨大(每代14%和18%)适应性代价的第二位点突变,创造了一种遗传背景,在这种背景下,链霉素敏感的rpsL + 等位基因相对于适应后的耐药菌株每代具有4 - 30%的选择性劣势。我们还提供证据表明,类似的补偿性突变在大肠杆菌长期链霉素耐药实验室菌株中已经固定下来,这可能解释了在没有抗生素的情况下维持超过10000代的种群中rpsL链霉素抗性的持续存在。我们讨论了这些以及其他实验结果对公共卫生的影响,这些结果质疑更谨慎地使用抗微生物化疗是否会导致耐药致病微生物发病率的下降。

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