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Control of Immunity by the Microbiota
Annual Review of Immunology ( IF 26.9 ) Pub Date : 2021-04-26 , DOI: 10.1146/annurev-immunol-093019-112348
Eduard Ansaldo 1 , Taylor K Farley 1, 2 , Yasmine Belkaid 1, 3
Affiliation  

The immune system has coevolved with extensive microbial communities living on barrier sites that are collectively known as the microbiota. It is increasingly clear that microbial antigens and metabolites engage in a constant dialogue with the immune system, leading to microbiota-specific immune responses that occur in the absence of inflammation. This form of homeostatic immunity encompasses many arms of immunity, including B cell responses, innate-like T cells, and conventional T helper and T regulatory responses. In this review we summarize known examples of innate-like T cell and adaptive immunity to the microbiota, focusing on fundamental aspects of commensal immune recognition across different barrier sites. Furthermore, we explore how this cross talk is established during development, emphasizing critical temporal windows that establish long-term immune function. Finally, we highlight how dysregulation of immunity to the microbiota can lead to inflammation and disease, and we pinpoint outstanding questions and controversies regarding immune system–microbiota interactions.

中文翻译:


微生物群对免疫的控制

免疫系统与生活在屏障位点上的广泛微生物群落共同进化,这些微生物群落统称为微生物群。越来越清楚的是,微生物抗原和代谢物与免疫系统不断对话,导致在没有炎症的情况下发生微生物群特异性免疫反应。这种形式的稳态免疫包括许多免疫臂,包括 B 细胞反应、先天样 T 细胞和常规 T 辅助和 T 调节反应。在这篇综述中,我们总结了已知的先天样 T 细胞和对微生物群的适应性免疫的例子,重点关注跨不同屏障位点的共生免疫识别的基本方面。此外,我们探索了这种串扰是如何在开发过程中建立的,强调建立长期免疫功能的关键时间窗口。最后,我们强调了对微生物群的免疫失调如何导致炎症和疾病,并指出了有关免疫系统-微生物群相互作用的突出问题和争议。

更新日期:2021-04-28
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