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The glial transcription factor Sox10 binds to DNA both as monomer and dimer with different functional consequences.

机译:神经胶质转录因子Sox10以单体和二聚体的形式结合到DNA上,具有不同的功能后果。

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Sox10 is an important transcriptional regulator in the neural crest and various neural-crest derived lineages, such as the Schwann cells of the peripheral nervous system. Recently, we identified the gene for myelin Protein zero (P(0)) as a transcriptional target of Sox10 in Schwann cells, allowing for the first time a detailed analysis of Sox10 responsive elements and their functional interaction with Sox10. Here we show that Sox10 functions through two different types of DNA response elements, one that allows binding of monomers, and a second that favors cooperative binding of two molecules. This dimeric binding required the presence of two heptameric Sox binding sites in a specific orientation and spacing, and was mediated by an N-terminal region of Sox10 with high conservation in the related Sox9, which also exhibited dimeric binding. This argues that the conserved region has the capacity to function as a DNA-dependent dimerization domain. The interaction between Sox10 dimers and DNA differed dramatically from that of Sox10 monomers, as it drastically reduced the protein's off-rate and increased the protein-induced angle of DNA bending. These results indicate that functionally relevant interactions between Sox10 and DNA occur through completely different modes of binding.
机译:Sox10是神经rest和各种神经rest衍生谱系(例如周围神经系统的雪旺氏细胞)中的重要转录调节因子。最近,我们确定了髓磷脂蛋白零(P(0))的基因作为Schwann细胞中Sox10的转录靶标,从而首次对Sox10响应元件及其与Sox10的功能相互作用进行了详细分析。在这里,我们显示Sox10通过两种不同类型的DNA反应元件起作用,一种允许单体结合,而第二种则有利于两个分子的协同结合。这种二聚体结合需要以特定的方向和间距存在两个七聚体Sox结合位点,并且由相关Sox9中具有高度保守性的Sox10的N端区域介导,该Sox9也表现出二聚体结合。这表明保守区具有充当依赖DNA的二聚化结构域的能力。 Sox10二聚体与DNA之间的相互作用与Sox10单体之间的相互作用显着不同,因为它大大降低了蛋白质的失活率,并增加了蛋白质诱导的DNA弯曲角度。这些结果表明,Sox10和DNA之间的功能相关相互作用是通过完全不同的结合方式发生的。

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