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首页> 外文期刊>Nature Genetics >X chromosome repression by localization of the C-elegans dosage compensation machinery to sites of transcription initiation
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X chromosome repression by localization of the C-elegans dosage compensation machinery to sites of transcription initiation

机译:通过将C-线虫剂量补偿机制定位到转录起始位点来抑制X染色体

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摘要

Among organisms with chromosome-based mechanisms of sex determination, failure to equalize expression of X-linked genes between the sexes is typically lethal. In C. elegans, XX hermaphrodites halve transcription from each X chromosome to match the output of XO males(1). Here, we mapped the binding location of the condensin homolog DPY-27 and the zinc finger protein SDC-3, two components of the C. elegans dosage compensation complex (DCC)(2,3). We observed strong foci of DCC binding on X, surrounded by broader regions of localization. Binding foci, but not adjacent regions of localization, were distinguished by clusters of a 10-bp DNA motif, suggesting a recruitment-and-spreading mechanism for X recognition. The DCC was preferentially bound upstream of genes, suggesting modulation of transcriptional initiation and polymerase-coupled spreading. Stronger DCC binding upstream of genes with high transcriptional activity indicated a mechanism for tuning DCC activity at specific loci. These data aid in understanding how proteins involved in higherorder chromosome dynamics can regulate transcription at individual loci.
机译:在具有基于染色体的性别决定机制的生物中,性别之间X连锁基因表达的均等化失败通常是致命的。在秀丽隐杆线虫中,XX个雌雄同体将每个X染色体的转录减半,以匹配XO雄性的输出(1)。在这里,我们绘制了凝缩素同系物DPY-27和锌指蛋白SDC-3(秀丽隐杆线虫剂量补偿复合物(DCC)(2,3)的两个组成部分)的结合位置。我们观察到DCC在X上有很强的结合力,被较宽的定位区域包围。结合的焦点,但不是本地化的相邻区域,通过10 bp DNA基序的簇来区分,表明X识别的募集和传播机制。 DCC优先绑定到基因的上游,表明转录起始和聚合酶偶联扩散的调节。具有高转录活性的基因上游较强的DCC结合表明在特定位点调节DCC活性的机制。这些数据有助于理解高阶染色体动力学中涉及的蛋白质如何调节单个基因座上的转录。

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