催产克雷伯菌
微生物学
生物
肺炎克雷伯菌
殖民地化
殖民抵抗
大肠杆菌
基因
遗传学
作者
Lisa Osbelt,Marie Wende,Neha Sahu,Elisabeth Derksen,Uthayakumar Muthukumarasamy,Till Robin Lesker,Eric J.C. Gálvez,Marina C. Pils,Enrico Schalk,Patrick Chhatwal,Jacqueline Färber,Meina Neumann‐Schaal,Thomas Fischer,Dirk Schlüter,Till Strowig
标识
DOI:10.1016/j.chom.2021.09.003
摘要
Gut colonization with multidrug-resistant (MDR) bacteria enhances the risk of bloodstream infections in susceptible individuals. We demonstrate highly variable degrees of ex vivo colonization resistance against a carbapenem-resistant Klebsiella pneumoniae strain in human feces samples and subsequently isolate diverse K. oxytoca strains from protected donors. Several of these K. oxytoca strains reduce gut colonization of MDR K. pneumoniae strains in antibiotic-treated and gnotobiotic mouse models. Comparative analysis of K. oxytoca strains coupled with CRISPR-Cas9-mediated deletion of casA, a protein essential for utilization of selected beta-glucosides, identified competition for specific carbohydrates as key in promoting colonization resistance. In addition to direct competition between K. oxytoca and K. pneumoniae, cooperation with additional commensals is required to reestablish full colonization resistance and gut decolonization. Finally, humanized microbiota mice generated from K. pneumoniae-susceptible donors are protected by K. oxytoca administration, demonstrating the potential of commensal K. oxytoca strains as next-generation probiotics.
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