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早期 T 细胞发育中 YY1 多梳蛋白家族蛋白功能的谱系特异性需求。

A lineage-specific requirement for YY1 Polycomb Group protein function in early T cell development.

机构信息

Department of Medical Sciences, School of Veterinary Medicine, University of Wisconsin, 2015 Linden Dr., Madison, WI 57306, USA.

Carbone Cancer Center, UW-Madison Blood Research Program, Madison, WI 53705, USA.

出版信息

Development. 2021 Apr 1;148(7). doi: 10.1242/dev.197319. Epub 2021 Apr 15.

Abstract

Yin Yang 1 (YY1) is a ubiquitous transcription factor and mammalian Polycomb Group protein (PcG) with important functions for regulating lymphocyte development and stem cell self-renewal. YY1 mediates stable PcG-dependent transcriptional repression via recruitment of PcG proteins that result in histone modifications. Many questions remain unanswered regarding how cell- and tissue-specificity is achieved by PcG proteins. Here, we demonstrate that a conditional knockout of Yy1 in the hematopoietic system results in an early T cell developmental blockage at the double negative (DN) 1 stage with reduced Notch1 signaling. There is a lineage-specific requirement for YY1 PcG function. YY1 PcG domain is required for T and B cell development but not necessary for myeloid cells. YY1 functions in early T cell development are multicomponent and involve both PcG-dependent and -independent regulations. Although YY1 promotes early T cell survival through its PcG function, its function to promote the DN1-to-DN2 transition and Notch1 expression and signaling is independent of its PcG function. Our results reveal how a ubiquitously expressed PcG protein mediates lineage-specific and context-specific functions to control early T cell development.

摘要

阴阳 1(YY1)是一种普遍存在的转录因子和哺乳动物多梳组蛋白(PcG),对于调节淋巴细胞发育和干细胞自我更新具有重要功能。YY1 通过募集导致组蛋白修饰的 PcG 蛋白来介导稳定的 PcG 依赖性转录抑制。关于 PcG 蛋白如何实现细胞和组织特异性,仍有许多问题尚未得到解答。在这里,我们证明了在造血系统中条件性敲除 Yy1 会导致 Notch1 信号降低,从而导致双阴性 (DN) 1 期早期 T 细胞发育阻滞。YY1 PcG 功能具有谱系特异性要求。YY1 PcG 结构域对于 T 和 B 细胞发育是必需的,但对于髓系细胞不是必需的。YY1 在早期 T 细胞发育中的功能是多组分的,涉及 PcG 依赖性和非依赖性调节。尽管 YY1 通过其 PcG 功能促进早期 T 细胞存活,但它促进 DN1 到 DN2 过渡以及 Notch1 表达和信号的功能与其 PcG 功能无关。我们的结果揭示了一种普遍表达的 PcG 蛋白如何介导谱系特异性和上下文特异性功能来控制早期 T 细胞发育。

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