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表观遗传学解释细胞分化的随机性:以T细胞分化和功能可塑性为例。

Stochastics of Cellular Differentiation Explained by Epigenetics: The Case of T-Cell Differentiation and Functional Plasticity.

作者信息

Bhat J, Helmuth J, Chitadze G, Kouakanou L, Peters C, Vingron M, Ammerpohl O, Kabelitz D

机构信息

Institute of Immunology, University of Kiel and University Hospital Schleswig-Holstein Campus Kiel, Kiel, Germany.

Otto-Warburg-Laboratories: Epigenomics, Max Planck Institute for Molecular Genetics, Berlin, Germany.

出版信息

Scand J Immunol. 2017 Oct;86(4):184-195. doi: 10.1111/sji.12589. Epub 2017 Sep 12.

DOI:10.1111/sji.12589
PMID:28799233
Abstract

Epigenetic marks including histone modifications and DNA methylation are associated with the regulation of gene expression and activity. In addition, an increasing number of non-coding RNAs with regulatory activity on gene expression have been identified. Alongside, technological advancements allow for the analysis of these mechanisms with high resolution up to the single-cell level. For instance, the assay for transposase-accessible chromatin using sequencing (ATAC-seq) simultaneously probes for chromatin accessibility and nucleosome positioning. Thus, it provides information on two levels of epigenetic regulation. Development and differentiation of T cells into functional subset cells including memory T cells are dynamic processes driven by environmental signals. Here, we briefly review the current knowledge of how epigenetic regulation contributes to subset specification, differentiation and memory development in T cells. Specifically, we focus on epigenetic mechanisms differentially active in the two distinct T cell populations expressing αβ or γδ T cell receptors. We also discuss examples of epigenetic alterations of T cells in autoimmune diseases. DNA methylation and histone acetylation are subject to modification by several classes of 'epigenetic modifiers', some of which are in clinical use or in preclinical development. Therefore, we address the impact of some epigenetic modifiers on T-cell activation and differentiation, and discuss possible synergies with T cell-based immunotherapeutic strategies.

摘要

包括组蛋白修饰和DNA甲基化在内的表观遗传标记与基因表达和活性的调控相关。此外,越来越多对基因表达具有调控活性的非编码RNA已被鉴定出来。与此同时,技术进步使得在单细胞水平上对这些机制进行高分辨率分析成为可能。例如,使用测序的转座酶可及染色质分析(ATAC-seq)可同时探测染色质可及性和核小体定位。因此,它提供了关于表观遗传调控两个层面的信息。T细胞发育和分化为包括记忆T细胞在内的功能性亚群细胞是由环境信号驱动的动态过程。在这里,我们简要回顾一下目前关于表观遗传调控如何促进T细胞亚群特化、分化和记忆发育的知识。具体而言,我们关注在表达αβ或γδT细胞受体的两种不同T细胞群体中差异活跃的表观遗传机制。我们还讨论了自身免疫性疾病中T细胞表观遗传改变的例子。DNA甲基化和组蛋白乙酰化会受到几类“表观遗传修饰剂”的修饰,其中一些正在临床使用或处于临床前开发阶段。因此,我们探讨了一些表观遗传修饰剂对T细胞活化和分化的影响,并讨论了与基于T细胞的免疫治疗策略可能存在的协同作用。

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