首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Role of CCCTC binding factor (CTCF) and cohesin in the generation of single-cell diversity of Protocadherin-oc gene expression
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Role of CCCTC binding factor (CTCF) and cohesin in the generation of single-cell diversity of Protocadherin-oc gene expression

机译:CCCTC结合因子(CTCF)和粘着蛋白在Protocadherin-oc基因表达的单细胞多样性产生中的作用

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摘要

Extraordinary single-cell diversity is generated in the vertebrate nervous system by the combinatorial expression of the clustered pro-tocadherin genes (Pcdhα, -β, and -γ). This diversity is generated by a combination of stochastic promoter choice and alternative pre-mRNA splicing. Here we show that both the insulator-binding protein CTCF and the cohesin complex subunit Rad21 bind to two highly conserved DNA sequences, the first within and the second downstream of transcriptionally active Pcdha promoters. Both CTCF and Rad21 bind to these sites in vitro and in vivo, this binding directly correlates with alternative isoform expression, and knocking'down CTCF expression reduces alternative isoform expression. Remarkably, a similarly spaced pair of CTCF/Rad21 binding sites was identified within a distant enhancer element (HS5-1), which is required for normal levels of alternative isoform expression. We also identify an additional, unique regulatory role for cohesin, as Rad21 binds to another enhancer (HS7) independently of CTCF, and knockdown of Rad21 reduces expression of the constitutive, biallelically expressed Pcdha isoforms ad and αc2. We propose that CTCF and the cohesin complex initiate and maintain Pcdha promoter choice by mediating interactions between Pcdhα promoters and enhancers.
机译:通过集群表达的前钙粘着蛋白基因(Pcdhα,-β和-γ)的组合表达,在脊椎动物神经系统中产生了非凡的单细胞多样性。这种多样性是通过随机启动子选择和替代性的预mRNA剪接相结合而产生的。在这里,我们显示绝缘子结合蛋白CTCF和黏附蛋白复合物Rad21亚基都结合到两个高度保守的DNA序列,即转录活性Pcdha启动子的第一个内部和第二个下游。 CTCF和Rad21在体外和体内均结合至这些位点,这种结合与备选同工型表达直接相关,并且敲低CTCF表达降低了备选同工型表达。值得注意的是,在远距离的增强子元件(HS5-1)中发现了一对类似间隔的CTCF / Rad21结合位点,这是正常水平的替代同工型表达所必需的。我们还确定了黏附蛋白的一个额外的,独特的调节作用,因为Rad21独立于CTCF与另一个增强子(HS7)结合,而敲除Rad21则减少了组成性,双烯丙基表达的Pcdha亚型ad和αc2的表达。我们建议CTCF和cohesin复杂通过介导Pcdhα启动子和增强子之间的相互作用来启动和维持Pcdha启动子的选择。

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