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细菌定植因子控制肠道微生物组的特异性和稳定性。

Bacterial colonization factors control specificity and stability of the gut microbiota.

机构信息

Division of Biology and Biological Engineering, California Institute of Technology, Pasadena, California 91125, USA.

出版信息

Nature. 2013 Sep 19;501(7467):426-9. doi: 10.1038/nature12447. Epub 2013 Aug 18.

Abstract

Mammals harbour a complex gut microbiome, comprising bacteria that confer immunological, metabolic and neurological benefits. Despite advances in sequence-based microbial profiling and myriad studies defining microbiome composition during health and disease, little is known about the molecular processes used by symbiotic bacteria to stably colonize the gastrointestinal tract. We sought to define how mammals assemble and maintain the Bacteroides, one of the most numerically prominent genera of the human microbiome. Here we find that, whereas the gut normally contains hundreds of bacterial species, germ-free mice mono-associated with a single Bacteroides species are resistant to colonization by the same, but not different, species. To identify bacterial mechanisms for species-specific saturable colonization, we devised an in vivo genetic screen and discovered a unique class of polysaccharide utilization loci that is conserved among intestinal Bacteroides. We named this genetic locus the commensal colonization factors (ccf). Deletion of the ccf genes in the model symbiont, Bacteroides fragilis, results in colonization defects in mice and reduced horizontal transmission. The ccf genes of B. fragilis are upregulated during gut colonization, preferentially at the colonic surface. When we visualize microbial biogeography within the colon, B. fragilis penetrates the colonic mucus and resides deep within crypt channels, whereas ccf mutants are defective in crypt association. Notably, the CCF system is required for B. fragilis colonization following microbiome disruption with Citrobacter rodentium infection or antibiotic treatment, suggesting that the niche within colonic crypts represents a reservoir for bacteria to maintain long-term colonization. These findings reveal that intestinal Bacteroides have evolved species-specific physical interactions with the host that mediate stable and resilient gut colonization, and the CCF system represents a novel molecular mechanism for symbiosis.

摘要

哺乳动物拥有复杂的肠道微生物群,其中包括赋予免疫、代谢和神经益处的细菌。尽管在基于序列的微生物分析技术取得了进展,并且有大量研究定义了健康和疾病期间微生物组的组成,但对于共生细菌用来稳定定植胃肠道的分子过程知之甚少。我们试图定义哺乳动物如何组装和维持拟杆菌,拟杆菌是人类微生物组中数量最多的属之一。在这里,我们发现,尽管肠道通常含有数百种细菌物种,但无菌小鼠单定植于单一拟杆菌物种时,对相同但不同物种的定植具有抗性。为了确定细菌进行种特异性可饱和定植的机制,我们设计了体内遗传筛选,并发现了一类独特的多糖利用基因座,该基因座在肠道拟杆菌中保守。我们将这个遗传基因座命名为共生定植因子(ccf)。在模式共生体脆弱拟杆菌中删除 ccf 基因,会导致小鼠定植缺陷和水平传播减少。ccf 基因在肠道拟杆菌中高度上调,在结肠表面更具优势。当我们在结肠内可视化微生物生物地理学时,脆弱拟杆菌穿透结肠黏液并存在于隐窝通道深处,而 ccf 突变体在隐窝关联方面存在缺陷。值得注意的是,在肠道微生物组被柠檬酸杆菌属 rodentium 感染或抗生素治疗破坏后,CCF 系统对于脆弱拟杆菌的定植是必需的,这表明结肠隐窝内的生态位代表了细菌维持长期定植的储备库。这些发现表明,肠道拟杆菌已经进化出与宿主的种特异性物理相互作用,介导稳定和有弹性的肠道定植,而 CCF 系统代表了共生的一种新的分子机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0ab1/3893107/6774cebd0616/nihms505094f1.jpg

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