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首页> 外文期刊>The journal of immunology >The Distal Upstream Promoter in Ly49 Genes, Pro1, Is Active in Mature NK Cells and T Cells, Does Not Require TATA Boxes, and Displays Enhancer Activity
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The Distal Upstream Promoter in Ly49 Genes, Pro1, Is Active in Mature NK Cells and T Cells, Does Not Require TATA Boxes, and Displays Enhancer Activity

机译:Ly49基因中的远端上游启动子Pro1在成熟的NK细胞和T细胞中活跃,不需要TATA盒,并显示增强子活性

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Missing self recognition of MHC class I molecules is mediated in murine species primarily through the stochastic expression of CD94/NKG2 and Ly49 receptors on NK cells. Previous studies have suggested that the stochastic expression of Ly49 receptors is achieved through the use of an alternate upstream promoter, designated Pro1, that is active only in immature NK cells and operates via the mutually exclusive binding of transcription initiation complexes to closely opposed forward and reverse TATA boxes, with forward transcription being transiently required to activate the downstream promoters, Pro2/Pro3, that are subsequently responsible for transcription in mature NK cells. In this study, we report that Pro1 transcripts are not restricted to immature NK cells but are also found in mature NK cells and T cells, and that Pro1 fragments display strong promoter activity in mature NK cell and T cell lines as well as in immature NK cells. However, the strength of promoter activity in vitro does not correlate well with Ly49 expression in vivo and forward promoter activity is generally weak or undetectable, suggesting that components outside of Pro1 are required for efficient forward transcription. Indeed, conserved sequences immediately upstream and downstream of the core Pro1 region were found to inhibit or enhance promoter activity. Most surprisingly, promoter activity does not require either the forward or reverse TATA boxes, but is instead dependent on residues in the largely invariant central region of Pro1. Importantly, Pro1 displays strong enhancer activity, suggesting that this may be its principal function in vivo.
机译:在鼠类中,主要通过CD94 / NKG2和Ly49受体在NK细胞上的随机表达来介导MHC I类分子的自我识别缺失。先前的研究表明,Ly49受体的随机表达是通过使用替代的上游启动子(称为Pro1)实现的,该启动子仅在未成熟的NK细胞中有活性,并通过转录起始复合物相互排斥的结合而紧密地对向和反向运动TATA盒需要暂时激活正向转录才能激活下游启动子Pro2 / Pro3,后者随后负责成熟NK细胞的转录。在这项研究中,我们报道Pro1转录本不仅限于未成熟的NK细胞,而且还存在于成熟的NK细胞和T细胞中,并且Pro1片段在成熟的NK细胞和T细胞系以及未成熟的NK中显示出强大的启动子活性。细胞。但是,体外启动子活性的强度与体内Ly49表达没有很好的相关性,并且正向启动子活性通常较弱或无法检测到,这表明有效正向转录需要Pro1以外的成分。实际上,发现核心Pro1区上游和下游的保守序列抑制或增强了启动子活性。最令人惊讶的是,启动子活性不需要正向或反向TATA盒,而是取决于Pro1的大部分不变中央区域中的残基。重要的是,Pro1显示出强大的增强子活性,表明这可能是其在体内的主要功能。

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