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肠道生物钟驱动微生物组维持胃肠道稳态。

The intestinal clock drives the microbiome to maintain gastrointestinal homeostasis.

机构信息

ZIEL - Institute for Food & Health, Technical University of Munich, 85354, Freising, Germany.

Chair of Nutrition and Immunology, Technical University of Munich, Gregor-Mendel-Str. 2, 85354, Freising, Germany.

出版信息

Nat Commun. 2022 Oct 14;13(1):6068. doi: 10.1038/s41467-022-33609-x.

Abstract

Diurnal (i.e., 24-hour) oscillations of the gut microbiome have been described in various species including mice and humans. However, the driving force behind these rhythms remains less clear. In this study, we differentiate between endogenous and exogenous time cues driving microbial rhythms. Our results demonstrate that fecal microbial oscillations are maintained in mice kept in the absence of light, supporting a role of the host's circadian system rather than representing a diurnal response to environmental changes. Intestinal epithelial cell-specific ablation of the core clock gene Bmal1 disrupts rhythmicity of microbiota. Targeted metabolomics functionally link intestinal clock-controlled bacteria to microbial-derived products, in particular branched-chain fatty acids and secondary bile acids. Microbiota transfer from intestinal clock-deficient mice into germ-free mice altered intestinal gene expression, enhanced lymphoid organ weights and suppressed immune cell recruitment. These results highlight the importance of functional intestinal clocks for microbiota composition and function, which is required to balance the host's gastrointestinal homeostasis.

摘要

肠道微生物组的昼夜(即 24 小时)波动在包括小鼠和人类在内的各种物种中都有描述。然而,这些节律背后的驱动力仍不太清楚。在这项研究中,我们区分了驱动微生物节律的内源性和外源性时间线索。我们的结果表明,在没有光照的情况下,粪便微生物的波动在小鼠中得以维持,这支持了宿主的生物钟系统的作用,而不是代表对环境变化的昼夜反应。肠道上皮细胞特异性敲除核心时钟基因 Bmal1 会破坏微生物群落的节律性。靶向代谢组学将肠道时钟控制的细菌与微生物衍生产物(特别是支链脂肪酸和次级胆汁酸)功能联系起来。从肠道时钟缺陷小鼠中转移的微生物群转移到无菌小鼠中,改变了肠道基因表达,增强了淋巴器官重量,并抑制了免疫细胞募集。这些结果强调了功能性肠道时钟对微生物群落组成和功能的重要性,这是平衡宿主胃肠道内稳态所必需的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/469b/9568547/dde42a8d860f/41467_2022_33609_Fig1_HTML.jpg

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