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在一项微观实验中,快速更换药物可减少细菌耐药性的演变。

Fast drug rotation reduces bacterial resistance evolution in a microcosm experiment.

作者信息

Zhou Dong-Hao, Zhang Quan-Guo

机构信息

State Key Laboratory of Earth Surface Processes and Resource Ecology and MOE Key Laboratory for Biodiversity Science and Ecological Engineering, College of Life Sciences, Beijing Normal University, Beijing, China.

出版信息

J Evol Biol. 2023 Apr;36(4):641-649. doi: 10.1111/jeb.14163. Epub 2023 Feb 19.

Abstract

Drug rotation (cycling), in which multiple drugs are administrated alternatively, has the potential for limiting resistance evolution in pathogens. The frequency of drug alternation could be a major factor to determine the effectiveness of drug rotation. Drug rotation practices often have low frequency of drug alternation, with an expectation of resistance reversion. Here we, based on evolutionary rescue and compensatory evolution theories, suggest that fast drug rotation can limit resistance evolution in the first place. This is because fast drug rotation would give little time for the evolutionarily rescued populations to recover in population size and genetic diversity, and thus decrease the chance of future evolutionary rescue under alternate environmental stresses. We experimentally tested this hypothesis using the bacterium Pseudomonas fluorescens and two antibiotics (chloramphenicol and rifampin). Increasing drug rotation frequency reduced the chance of evolutionary rescue, and most of the finally surviving bacterial populations were resistant to both drugs. Drug resistance incurred significant fitness costs, which did not differ among the drug treatment histories. A link between population sizes during the early stages of drug treatment and the end-point fates of populations (extinction vs survival) suggested that population size recovery and compensatory evolution before drug shift increase the chance of population survival. Our results therefore advocate fast drug rotation as a promising approach to reduce bacterial resistance evolution, which in particular could be a substitute for drug combination when the latter has safety risks.

摘要

药物轮换(循环用药),即交替使用多种药物,有可能限制病原体耐药性的演变。药物交替的频率可能是决定药物轮换有效性的一个主要因素。药物轮换实践中的药物交替频率往往较低,期望实现耐药性逆转。在此,基于进化救援和补偿进化理论,我们认为快速药物轮换首先可以限制耐药性的演变。这是因为快速药物轮换几乎不给进化救援后的种群留出时间来恢复种群数量和遗传多样性,从而降低在交替环境压力下未来进行进化救援的机会。我们使用荧光假单胞菌和两种抗生素(氯霉素和利福平)对这一假设进行了实验验证。提高药物轮换频率降低了进化救援的机会,并且大多数最终存活的细菌种群对两种药物都具有耐药性。耐药性带来了显著的适合度代价,在不同的药物治疗历程中这一代价并无差异。药物治疗早期阶段的种群数量与种群的最终命运(灭绝与存活)之间的联系表明,在药物更换之前种群数量的恢复和补偿进化会增加种群存活的机会。因此,我们的研究结果主张将快速药物轮换作为一种有前景的减少细菌耐药性演变的方法,特别是在药物联合使用存在安全风险时,它尤其可以作为药物联合使用的替代方法。

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