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细胞因子介导的肠道黏膜免疫中固有淋巴细胞可塑性的调节。

Cytokine-Mediated Regulation of Innate Lymphoid Cell Plasticity in Gut Mucosal Immunity.

机构信息

Department of Pathology, Case Western Reserve University School of Medicine, Cleveland, OH, United States.

出版信息

Front Immunol. 2020 Dec 4;11:585319. doi: 10.3389/fimmu.2020.585319. eCollection 2020.

Abstract

Mucosal barriers are active sites that encounter a bombardment of antigenic stimuli derived from both the commensal flora and a variety of pathogens, as well as from environmental insults. As such, the ability to mount appropriate innate immune responses is an important first line of defense that confers protection to the host. Central to innate immunity are innate lymphoid cells (ILCs), which were first described a decade ago, and represent a family of heterogeneous cells driven by specific transcription factors and exhibit distinct cytokine profiles that are shared with their CD4 T-helper cell counterparts. ILCs are particularly enriched at mucosal surfaces, and the tissue microenvironment and cytokine milieu in which ILCs reside are critical factors that drive the behavior and overall function of these cells. In fact, ILCs situated at mucosal barriers must be able to temper their response to a constant exposure of environmental antigens, but also promptly react to pathogens or signals that are potentially harmful to the host. In this context, the ability of ILCs to readily transdifferentiate in response to their dynamic surroundings has become a vigorous area of research, and defining specific mechanism(s) of ILC plasticity is at the advent of discovery. This review will summarize what is currently known regarding the network of cytokines and regulatory elements that enable ILCs to readily transform, based on the range of diverse signals and signal gradients they encounter that lead to either protective or pathogenic function(s), with focus on the gut mucosal immune system.

摘要

黏膜屏障是一个活性部位,会接触到来自共生菌群和各种病原体以及环境侵袭的抗原刺激。因此,能够引发适当的先天免疫反应是宿主提供保护的第一道重要防线。先天免疫的核心是先天淋巴细胞(ILC),它们在十年前首次被描述,代表了一组由特定转录因子驱动的异质性细胞,表现出与 CD4 T 辅助细胞相似的独特细胞因子谱。ILC 特别丰富地存在于黏膜表面,而 ILC 所在的组织微环境和细胞因子环境是驱动这些细胞行为和整体功能的关键因素。事实上,位于黏膜屏障的 ILC 必须能够调节其对环境抗原持续暴露的反应,但也要迅速对可能对宿主有害的病原体或信号做出反应。在这种情况下,ILC 能够根据其动态环境迅速转分化的能力已成为一个活跃的研究领域,并且确定 ILC 可塑性的特定机制正处于发现的前沿。本综述将总结目前已知的细胞因子和调节因子网络,这些网络使 ILC 能够根据其遇到的导致保护或致病功能的各种信号和信号梯度,迅速转化,重点关注肠道黏膜免疫系统。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e337/7794016/5733b740469b/fimmu-11-585319-g001.jpg

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