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首页> 外文期刊>Nucleic Acids Research >Distinct transcriptional regulatory modules underlie STAT3's cell type-independent and cell type-specific functions
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Distinct transcriptional regulatory modules underlie STAT3's cell type-independent and cell type-specific functions

机译:STAT3的独立于细胞类型和特定于细胞类型的功能是不同的转录调控模块

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摘要

Transcription factors (TFs) regulate gene expression by binding to short DNA sequence motifs, yet their binding specificities alone cannot explain how certain TFs drive a diversity of biological processes. In order to investigate the factors that control the functions of the pleiotropic TF STAT3, we studied its genome-wide binding patterns in four different cell types: embryonic stem cells, CD4+ T cells, macrophages and AtT-20 cells. We describe for the first time two distinct modes of STAT3 binding.First, a small cell type-independent mode represented by a set of 35 evolutionarily conserved STAT3-binding sites that collectively regulate STAT3's own functions and cell growth. We show that STAT3 is recruited to sites with E2F1 already pre-bound before STATS activation. Second, a series of different transcriptional regulatory modules (TRMs) assemble around STAT3 to drive distinct transcriptional programs in the four cell types. These modules recognize cell type-specific binding sites and are associated with factors particular to each cell type. Our study illustrates the versatility of STAT3 to regulate both universal- and cell type-specific functions by means of distinct TRMs, a mechanism that might be common to other pleiotropic TFs.
机译:转录因子(TFs)通过与短的DNA序列基序结合来调节基因表达,但是它们的结合特异性本身不能解释某些TF如何驱动多种生物过程。为了研究控制多效性TF STAT3功能的因素,我们研究了四种不同细胞类型的全基因组结合模式:胚胎干细胞,CD4 + T细胞,巨噬细胞和AtT-20细胞。我们首次描述了STAT3结合的两种不同模式:首先,一种由35个进化保守的STAT3结合位点代表的小细胞类型独立模式,它们共同调节STAT3自身的功能和细胞生长。我们显示STAT3被招募到在STATS激活之前已预先绑定E2F1的站点。其次,在STAT3周围组装了一系列不同的转录调控模块(TRM),以驱动四种细胞类型中不同的转录程序。这些模块识别细胞类型特异性结合位点,并与每种细胞类型特有的因子相关。我们的研究表明,STAT3可以通过不同的TRM来调节通用和特定于细胞类型的功能,这是其他多效TF可能共有的机制。

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