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负责调节CD4(+)外周T淋巴细胞中T细胞受体β/CD4以及白细胞介素-4/干扰素-γ表达的Runx1转录因子的结构域分析。

Domain analyses of the Runx1 transcription factor responsible for modulating T-cell receptor-beta/CD4 and interleukin-4/interferon-gamma expression in CD4(+) peripheral T lymphocytes.

作者信息

Uchino Ryuji

机构信息

Department of Molecular Immunology, Institute of Development, Aging and Cancer, Graduate School of Life Science, Tohoku University, Sendai, Japan.

出版信息

Immunology. 2009 Sep;128(1):16-24. doi: 10.1111/j.1365-2567.2009.03042.x.

Abstract

The Runx1 transcription factor is one of the master regulators of T-lymphocyte differentiation. There have been several reports trying to assign a domain within the Runx1 protein that is responsible for gene expression in thymocytes. The Runx1 domains involved in regulating the expression of several genes in peripheral CD4(+) T cells were analysed. It was observed that Runx1 over-expression enhanced the surface expression of CD4 and CD69 molecules via its activation domain and VWRPY domain, and decreased that of T-cell receptor-beta via its activation domain. Runx1 over-expression enhanced interferon-gamma expression via its activation and VWRPY domains, and abolished interleukin-4 expression through its activation domain. Transduction of Runx1 did not down-regulate CD4 expression until 72 hr of culture, but the repression of CD4 expression became evident after 96 hr. The main region responsible for repressing CD4 expression was the inhibitory domain of Runx1. Taken together, these results lead to a proposal that the regions in Runx1 responsible for modulating gene expression are distinct in thymocytes and in peripheral CD4(+) T cells.

摘要

Runx1转录因子是T淋巴细胞分化的主要调节因子之一。已有多篇报道试图确定Runx1蛋白中负责胸腺细胞基因表达的结构域。对参与调节外周CD4(+) T细胞中多个基因表达的Runx1结构域进行了分析。结果发现,Runx1过表达通过其激活结构域和VWRPY结构域增强了CD4和CD69分子的表面表达,而通过其激活结构域降低了T细胞受体β的表达。Runx1过表达通过其激活结构域和VWRPY结构域增强了干扰素-γ的表达,并通过其激活结构域消除了白细胞介素-4的表达。Runx1的转导在培养72小时后才下调CD4表达,但在96小时后CD4表达的抑制变得明显。负责抑制CD4表达的主要区域是Runx1的抑制结构域。综上所述,这些结果表明,Runx1中负责调节基因表达的区域在胸腺细胞和外周CD4(+) T细胞中是不同的。

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