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几十年来放松选择后抗生素耐药性演变中的历史偶然性。

Historical contingency in the evolution of antibiotic resistance after decades of relaxed selection.

机构信息

BEACON Center for the Study of Evolution in Action, Michigan State University, East Lansing, Michigan, United States of America.

Department of Microbiology and Molecular Genetics, Michigan State University, East Lansing, Michigan, United States of America.

出版信息

PLoS Biol. 2019 Oct 23;17(10):e3000397. doi: 10.1371/journal.pbio.3000397. eCollection 2019 Oct.

Abstract

Populations often encounter changed environments that remove selection for the maintenance of particular phenotypic traits. The resulting genetic decay of those traits under relaxed selection reduces an organism's fitness in its prior environment. However, whether and how such decay alters the subsequent evolvability of a population upon restoration of selection for a previously diminished trait is not well understood. We addressed this question using Escherichia coli strains from the long-term evolution experiment (LTEE) that independently evolved for multiple decades in the absence of antibiotics. We first confirmed that these derived strains are typically more sensitive to various antibiotics than their common ancestor. We then subjected the ancestral and derived strains to various concentrations of these drugs to examine their potential to evolve increased resistance. We found that evolvability was idiosyncratic with respect to initial genotype; that is, the derived strains did not generally compensate for their greater susceptibility by "catching up" to the resistance level of the ancestor. Instead, the capacity to evolve increased resistance was constrained in some backgrounds, implying that evolvability depended upon prior mutations in a historically contingent fashion. We further subjected a time series of clones from one LTEE population to tetracycline and determined that an evolutionary constraint arose early in that population, corroborating the role of contingency. In summary, relaxed selection not only can drive populations to increased antibiotic susceptibility, but it can also affect the subsequent evolvability of antibiotic resistance in an unpredictable manner. This conclusion has potential implications for public health, and it underscores the need to consider the genetic context of pathogens when designing drug-treatment strategies.

摘要

生物种群常常会遇到改变了的环境,这些环境消除了对特定表型特征的选择。在放松选择的情况下,这些特征的遗传衰退会降低生物体在其先前环境中的适应度。然而,在选择恢复对先前减少的特征的情况下,这种衰退是否以及如何改变种群的后续可进化性,目前还不是很清楚。我们使用来自长期进化实验(LTEE)的大肠杆菌菌株来解决这个问题,这些菌株在没有抗生素的情况下独立进化了几十年。我们首先证实,这些衍生菌株通常比它们的共同祖先对各种抗生素更敏感。然后,我们将祖先和衍生菌株暴露于不同浓度的这些药物中,以研究它们进化出更高抗性的潜力。我们发现,可进化性与初始基因型有关;也就是说,衍生菌株并没有通过“赶上”祖先的抗性水平来普遍弥补它们更高的敏感性。相反,在某些背景下,进化出更高抗性的能力受到限制,这意味着可进化性依赖于历史上偶然的先前突变。我们进一步对一个 LTEE 种群的一个时间序列的克隆进行了四环素处理,并确定在该种群中早期出现了进化约束,这证实了偶然性的作用。总之,放松选择不仅可以使种群对抗生素的敏感性增加,而且还可以以不可预测的方式影响抗生素抗性的后续可进化性。这个结论对公共卫生有潜在的影响,它强调了在设计药物治疗策略时需要考虑病原体的遗传背景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/808d/6827916/8f884f0ea82c/pbio.3000397.g001.jpg

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