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Rapid evolution drives the rise and fall of carbapenem resistance during an acute Pseudomonas aeruginosa infection

 
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Manage episode 288621295 series 2902310
内容由MultiModal LLC and Multimodal LLC提供。所有播客内容(包括剧集、图形和播客描述)均由 MultiModal LLC and Multimodal LLC 或其播客平台合作伙伴直接上传和提供。如果您认为有人在未经您许可的情况下使用您的受版权保护的作品,您可以按照此处概述的流程进行操作https://zh.player.fm/legal
Link to bioRxiv paper: http://biorxiv.org/cgi/content/short/2020.08.10.243741v1?rss=1 Authors: Wheatley, R., Diaz Caballero, J., Kapel, N., Quinn, A., del Barrio-Tofino, E., Lopez-Causape, C., Hedge, J., Torrens, G., Van der Schalk, T., Britto Xavier, B., Fernandez-Cuenca, F., Arenzana, A., Recanatini, C., Timbermont, L., Sifakis, F., Ruzin, A., Ali, O., Lammens, C., Goossens, H., Kluytmans, J., Kumar-Singh, S., Oliver, A., Malhotra-Kumar, S., MacLean, C. Abstract: It is well established that antibiotic treatment selects for resistance in pathogenic bacteria. However, the evolutionary responses of pathogen populations to antibiotic treatment during infections remain poorly resolved, especially in acute infections. Here we map the evolutionary responses to treatment in high definition through genomic and phenotypic characterization of >100 isolates from a patient with P. aeruginosa pneumonia. Antibiotic therapy (meropenem, colistin) caused a rapid crash of the P. aeruginosa population in the lung, but this decline was followed by the spread of meropenem resistance mutations that restrict antibiotic uptake (oprD) or modify LPS biosynthesis (wbpM). Low fitness strains with high-level meropenem resistance (oprD) were then replaced by high fitness strains with 'anti-resistance' mutations in the MexAB-OprM efflux pump, causing a rapid decline in resistance to both meropenem and a collateral loss of resistance to a broad spectrum of antibiotics. In contrast, we did not observe any evolutionary responses to antibiotic treatment in the intestinal population of P. aeruginosa. Carbapenem antibiotics are key to the treatment of infections caused by Gram negative pathogens, and our work highlights the ability of natural selection to drive both the rapid rise and fall of carbapenem resistance during acute infections. Copy rights belong to original authors. Visit the link for more info
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已归档的系列专辑 ("不活跃的收取点" status)

When? This feed was archived on December 15, 2021 15:07 (2+ y ago). Last successful fetch was on March 29, 2021 12:55 (3y ago)

Why? 不活跃的收取点 status. 我们的伺服器已尝试了一段时间,但仍然无法截取有效的播客收取点

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Manage episode 288621295 series 2902310
内容由MultiModal LLC and Multimodal LLC提供。所有播客内容(包括剧集、图形和播客描述)均由 MultiModal LLC and Multimodal LLC 或其播客平台合作伙伴直接上传和提供。如果您认为有人在未经您许可的情况下使用您的受版权保护的作品,您可以按照此处概述的流程进行操作https://zh.player.fm/legal
Link to bioRxiv paper: http://biorxiv.org/cgi/content/short/2020.08.10.243741v1?rss=1 Authors: Wheatley, R., Diaz Caballero, J., Kapel, N., Quinn, A., del Barrio-Tofino, E., Lopez-Causape, C., Hedge, J., Torrens, G., Van der Schalk, T., Britto Xavier, B., Fernandez-Cuenca, F., Arenzana, A., Recanatini, C., Timbermont, L., Sifakis, F., Ruzin, A., Ali, O., Lammens, C., Goossens, H., Kluytmans, J., Kumar-Singh, S., Oliver, A., Malhotra-Kumar, S., MacLean, C. Abstract: It is well established that antibiotic treatment selects for resistance in pathogenic bacteria. However, the evolutionary responses of pathogen populations to antibiotic treatment during infections remain poorly resolved, especially in acute infections. Here we map the evolutionary responses to treatment in high definition through genomic and phenotypic characterization of >100 isolates from a patient with P. aeruginosa pneumonia. Antibiotic therapy (meropenem, colistin) caused a rapid crash of the P. aeruginosa population in the lung, but this decline was followed by the spread of meropenem resistance mutations that restrict antibiotic uptake (oprD) or modify LPS biosynthesis (wbpM). Low fitness strains with high-level meropenem resistance (oprD) were then replaced by high fitness strains with 'anti-resistance' mutations in the MexAB-OprM efflux pump, causing a rapid decline in resistance to both meropenem and a collateral loss of resistance to a broad spectrum of antibiotics. In contrast, we did not observe any evolutionary responses to antibiotic treatment in the intestinal population of P. aeruginosa. Carbapenem antibiotics are key to the treatment of infections caused by Gram negative pathogens, and our work highlights the ability of natural selection to drive both the rapid rise and fall of carbapenem resistance during acute infections. Copy rights belong to original authors. Visit the link for more info
  continue reading

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