Hypervirulent Klebsiella pneumoniae employs genomic island encoded toxins against bacterial competitors in the gut.

IF 10.8 1区 环境科学与生态学 Q1 ECOLOGY ISME Journal Pub Date : 2024-01-08 DOI:10.1093/ismejo/wrae054
Yi Han Tan, Patricio Arros, Camilo Berríos-Pastén, Indrik Wijaya, Wilson H W Chu, Yahua Chen, Guoxiang Cheam, Ahmad Nazri Mohamed Naim, Andrés E Marcoleta, Aarthi Ravikrishnan, Niranjan Nagarajan, Rosalba Lagos, Yunn-Hwen Gan
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Abstract

The hypervirulent lineages of Klebsiella pneumoniae (HvKp) cause invasive infections such as Klebsiella-liver abscess. Invasive infection often occurs after initial colonization of the host gastrointestinal tract by HvKp. Over 80% of HvKp isolates belong to the clonal group 23 sublineage I that has acquired genomic islands (GIs) GIE492 and ICEKp10. Our analysis of 12 361 K. pneumoniae genomes revealed that GIs GIE492 and ICEKp10 are co-associated with the CG23-I and CG10118 HvKp lineages. GIE492 and ICEKp10 enable HvKp to make a functional bacteriocin microcin E492 (mccE492) and the genotoxin colibactin, respectively. We discovered that GIE492 and ICEKp10 play cooperative roles and enhance gastrointestinal colonization by HvKp. Colibactin is the primary driver of this effect, modifying gut microbiome diversity. Our in vitro assays demonstrate that colibactin and mccE492 kill or inhibit a range of Gram-negative Klebsiella species and Escherichia coli strains, including Gram-positive bacteria, sometimes cooperatively. Moreover, mccE492 and colibactin kill human anaerobic gut commensals that are similar to the taxa found altered by colibactin in the mouse intestines. Our findings suggest that GIs GIE492 and ICEKp10 enable HvKp to kill several commensal bacterial taxa during interspecies interactions in the gut. Thus, acquisition of GIE492 and ICEKp10 could enable better carriage in host populations and explain the dominance of the CG23-I HvKp lineage.

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超病毒性肺炎克雷伯氏菌利用基因组岛编码的毒素对付肠道中的细菌竞争者。
肺炎克雷伯氏菌(Klebsiella pneumoniae,HvKp)的高脓毒性菌系可引起侵袭性感染,如肝脏脓肿(Klebsiella-liver abscess)。入侵性感染通常发生在 HvKp 最初在宿主胃肠道定植之后。超过 80% 的 HvKp 分离物属于获得了基因组岛 GIE492 和 ICEKp10 的 23 亚系 I 克隆组。我们对 12,361 个肺炎克氏菌基因组的分析表明,基因组岛 GIE492 和 ICEKp10 与 CG23-I 和 CG10118 HvKp 支系共同相关。GIE492 和 ICEKp10 使 HvKp 能够分别制造功能性细菌素 microcin E492(mccE492)和基因毒素 colibactin。我们发现,GIE492 和 ICEKp10 发挥着协同作用,并增强了 HvKp 在胃肠道的定植。可乐菌素是这种效应的主要驱动因素,它改变了肠道微生物群的多样性。我们的体外试验表明,可乐菌素和 mccE492 能杀死或抑制一系列革兰氏阴性克雷伯氏菌和大肠杆菌菌株,包括革兰氏阳性菌,有时还能协同作用。此外,mccE492 和可乐菌素还能杀死人类肠道厌氧共生菌,这些厌氧共生菌与小鼠肠道中被可乐菌素改变的类群相似。我们的研究结果表明,基因组岛 GIE492 和 ICEKp10 使 HvKp 能够在肠道内的种间相互作用中杀死多种共生细菌类群。因此,获得 GIE492 和 ICEKp10 可使 HvKp 在宿主群体中更好地携带,并解释 CG23-I HvKp 系的优势。
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来源期刊
ISME Journal
ISME Journal 环境科学-生态学
CiteScore
22.10
自引率
2.70%
发文量
171
审稿时长
2.6 months
期刊介绍: The ISME Journal covers the diverse and integrated areas of microbial ecology. We encourage contributions that represent major advances for the study of microbial ecosystems, communities, and interactions of microorganisms in the environment. Articles in The ISME Journal describe pioneering discoveries of wide appeal that enhance our understanding of functional and mechanistic relationships among microorganisms, their communities, and their habitats.
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