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小鼠CBFalpha2基因干细胞启动子的表达与功能:在自然杀伤细胞和T细胞发育中的不同作用及调控

Expression and function of a stem cell promoter for the murine CBFalpha2 gene: distinct roles and regulation in natural killer and T cell development.

作者信息

Telfer J C, Rothenberg E V

机构信息

Division of Biology, California Institute of Technology, Pasadena 91125, USA.

出版信息

Dev Biol. 2001 Jan 15;229(2):363-82. doi: 10.1006/dbio.2000.9991.

Abstract

The Runt family transcription factor CBFalpha2 (AML1, PEBP2alphaB, or Runx1) is required by hematopoietic stem cells and expressed at high levels in T-lineage cells. In human T cells CBFalpha2 is usually transcribed from a different promoter (distal promoter) than in myeloid cells (proximal promoter), but the developmental and functional significance of this promoter switch has not been known. Here, we report that both coding and noncoding sequences of the distal 5' end are highly conserved between the human and the murine genes, and the distal promoter is responsible for the overwhelming majority of CBFalpha2 expression in murine hematopoietic stem cells as well as in T cells. Distal promoter activity is maintained throughout T cell development and at lower levels in B cell development, but downregulated in natural killer cell development. The distal N-terminal isoform binds to functionally important regulatory sites from known target genes with two- to threefold higher affinity than the proximal N-terminal isoform. Neither full-length isoform alters growth of a myeloid cell line under nondifferentiating conditions, but the proximal isoform selectively delays mitotic arrest of the cell line under differentiating conditions, resulting in the generation of greater numbers of neutrophils.

摘要

Runt家族转录因子CBFα2(AML1、PEBP2αB或Runx1)是造血干细胞所必需的,并且在T细胞系中高水平表达。在人类T细胞中,CBFα2通常从与髓系细胞(近端启动子)不同的启动子(远端启动子)转录而来,但这种启动子切换的发育和功能意义尚不清楚。在此,我们报道人类和鼠类基因的远端5'端的编码和非编码序列都高度保守,并且远端启动子负责鼠类造血干细胞以及T细胞中绝大多数CBFα2的表达。远端启动子活性在整个T细胞发育过程中得以维持,在B细胞发育过程中活性较低,但在自然杀伤细胞发育过程中被下调。远端N末端异构体与已知靶基因的功能重要调控位点结合,其亲和力比近端N末端异构体高两到三倍。在未分化条件下,两种全长异构体均不改变髓系细胞系的生长,但在分化条件下,近端异构体选择性地延迟细胞系的有丝分裂停滞,从而导致产生更多的中性粒细胞。

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