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调节性 T 细胞在 1 型糖尿病中的功能、衰竭和未来潜力。

Function, Failure, and the Future Potential of Tregs in Type 1 Diabetes.

机构信息

Division of Microbiology and Immunology, Department of Pathology, University of Utah, Salt Lake City, UT

出版信息

Diabetes. 2021 Jun;70(6):1211-1219. doi: 10.2337/dbi18-0058. Epub 2021 May 20.

Abstract

Critical insights into the etiology of type 1 diabetes (T1D) came from genome-wide association studies that unequivocally connected genetic susceptibility to immune cell function. At the top of the susceptibility are genes involved in regulatory T-cell (Treg) function and development. The advances in epigenetic and transcriptional analyses have provided increasing evidence for Treg dysfunction in T1D. These are well supported by functional studies in mouse models and analysis of peripheral blood during T1D. For these reasons, Treg-based therapies are at the forefront of research and development and have a tangible probability to deliver a long-sought-after successful immune-targeted treatment for T1D. The current challenge in the field is whether we can directly assess Treg function at the tissue site or make informative interpretations based on peripheral data. Future studies focused on Treg function in pancreatic lymph nodes and pancreas could provide key insight into the ultimate mechanisms underlying Treg failure in T1D. In this Perspective we will provide an overview of current literature regarding Treg development and function in T1D and how this knowledge has been applied to Treg therapies.

摘要

对 1 型糖尿病 (T1D) 病因的深入了解来自全基因组关联研究,这些研究明确将遗传易感性与免疫细胞功能联系起来。易感性的首要因素是涉及调节性 T 细胞 (Treg) 功能和发育的基因。表观遗传和转录分析的进展为 T1D 中的 Treg 功能障碍提供了越来越多的证据。这些证据得到了小鼠模型中的功能研究和 T1D 期间外周血分析的很好支持。由于这些原因,基于 Treg 的疗法处于研究和开发的前沿,并且有可能为 T1D 提供长期以来寻求的成功的免疫靶向治疗。该领域目前的挑战是我们是否可以直接在组织部位评估 Treg 功能,或者基于外周数据进行有意义的解释。未来专注于胰腺淋巴结和胰腺中 Treg 功能的研究可能会为 T1D 中 Treg 失败的最终机制提供关键见解。在本观点中,我们将概述关于 T1D 中 Treg 发育和功能的当前文献,以及如何将这些知识应用于 Treg 疗法。

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