人类肠道微生物群内的自诱导剂-2介导的通讯网络

Qingying Fan, Hengxi Sun, Xueyuan Lin, Wenguang Yang, Xihui Shen, Lei Zhang
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摘要

群体感应(Quorum sensing, QS)是一种将不同微生物系统中的微生物成员连接起来的化学通讯过程。由QS介导的细菌通讯网络在调节宿主肠道微生态平衡及营养代谢等方面发挥着重要作用。然而,人类肠道微生物如何利用QS信号相互交流在很大程度上仍然未知。在这项研究中,我们首先检测了编码QS信号合成酶基因的基因的流行度和丰度,这些基因来自统一人类胃肠道基因组收集的289232个原核生物基因组中的3329个物种代表。我们的研究结果表明,AI-2是人类肠道微生物群中最普遍的QS信号,合成酶基因luxS在2039个物种中被发现,主要分布在厚壁菌门、放线菌门、拟杆菌门和变形菌门。此外,299种植物携带编码一种或多种AI-2受体的基因(LuxP-、LsrB-、dCache_1-和gapes1型)。dCache_1-和gapes1型受体可作为甲基化趋化蛋白、组氨酸激酶、c-di-GMP合成酶和/或c-di-GMP特异性磷酸二酯酶、丝氨酸磷酸酶和丝氨酸/苏氨酸激酶,提示ai -2介导的人类肠道微生物群间交流模式的多样性。超转录组学分析显示,在健康和/或不健康状态下,许多AI-2合成酶和受体编码基因可以在人类肠道中表达。通信网络分析表明,ai -2介导的相互作用广泛发生在厚壁菌门、变形菌门、放线菌门、弯曲菌门和螺旋体菌门的成员之间。综上所述,本研究加深了对人类肠道菌群间qs介导的通讯网络的理解,为肠道菌群工程化和基于复杂微生物相互作用构建新的合成菌群提供了指导。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Autoinducer-2-mediated communication network within human gut microbiota
Quorum sensing (QS) is a chemical communication process that connects microbial members in various microbial systems. Bacterial communication networks mediated by QS play important roles in the regulation of intestinal microecological balance as well as nutrition and metabolism of the host. However, how human gut microbes utilize QS signals to communicate with one another remains largely unknown. In this study, we first examined the prevalence and abundance of genes encoding QS signal synthases in 3329 species representatives clustered from 289232 prokaryotic genomes in the Unified Human Gastrointestinal Genome collection. Our results show autoinducer-2 (AI-2) is the most prevalent QS signal within the human gut microbiota, with the synthase gene luxS being found in 2039 species mainly distributed within Firmicutes, Actinobacteriota, Bacteroidota, and Proteobacteria. Furthermore, 299 species carry genes encoding one or more types of AI-2 receptors (LuxP-, LsrB-, dCache_1-, and GAPES1-type). The dCache_1- and GAPES1-type receptors can function as methyl-accepting chemotaxis proteins, histidine kinases, c-di-GMP synthases and/or c-di-GMP-specific phosphodiesterases, serine phosphatases, and serine/threonine kinases, suggesting the diversity of AI-2-mediated interspecies communication modes among human gut microbiota. Metatranscriptomic analysis showed that a number of AI-2 synthase- and receptor-encoding genes can be expressed in the human gut in healthy and/or unhealthy states. The communication network analysis suggests that AI-2-mediated interactions widely occur among members of Firmicutes, Proteobacteria, Actinobacteriota, Campylobacterota, and Spirochaetota. Overall, this study deepens understanding of QS-mediated communication network among human gut microbiota, and provides guidance for engineering gut microbiota and constructing new synthetic microbial consortia based on complex microbial interactions.
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