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A domain of the even-skipped protein represses transcription by preventing TFIID binding to a promoter: repression by cooperative blocking.

机译:通过阻止TFIID与启动子结合,均匀跳过蛋白的结构域可抑制转录:通过协同阻断来抑制。

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We examined the mechanism by which the C-terminal 236 amino acids of the even-skipped protein (region CD) repress transcription. A fusion protein, CDGB, was created that contains region CD fused to the glucocorticoid receptor DNA binding domain. This protein repressed transcription in an in vitro system containing purified fractions of the RNA polymerase II general transcription factors, and repression was dependent upon the presence of high-affinity glucocorticoid receptor binding sites in the promoter. Repression by CDGB was prevented when the promoter DNA was preincubated with TFIID or TBP, whereas preincubation of the template DNA with CDGB prevented TFIID binding. Together, these results strongly imply that CDGB represses transcription by inhibiting TFIID binding, and further experiments suggested a mechanism by which this may occur. Region CD can mediate cooperative interactions between repressor molecules such that molecules bound at the glucocorticoid receptor binding sites stabilize binding of additional CDGB molecules to low-affinity binding sites throughout the basal promoter. Binding to some of these low-affinity sites was shown to contribute to repression. Further experiments suggested that the full-length eve protein also represses transcription by the same mechanism. We speculate that occupancy of secondary sites within the basal promoter by CDGB or the eve protein inhibits subsequent TFIID binding to repress transcription, a mechanism we term cooperative blocking.
机译:我们检查了均匀跳过的蛋白质(区域CD)的C端236个氨基酸抑制转录的机制。创建了融合蛋白CDGB,其包含与糖皮质激素受体DNA结合域融合的区域CD。该蛋白在包含RNA聚合酶II一般转录因子纯化部分的体外系统中抑制转录,并且抑制取决于启动子中高亲和力糖皮质激素受体结合位点的存在。当将启动子DNA与TFIID或TBP预孵育时,可防止CDGB抑制,而将模板DNA与CDGB的预孵育可防止TFIID结合。总之,这些结果强烈暗示CDGB通过抑制TFIID结合来抑制转录,进一步的实验表明了这种机制可能会发生。 CD区域可以介导阻遏物分子之间的协同相互作用,从而使糖皮质激素受体结合位点处结合的分子稳定其他CDGB分子与整个基础启动子中低亲和力结合位点的结合。已显示与这些低亲和力位点的某些结合有助于抑制。进一步的实验表明全长eve蛋白也通过相同的机制抑制转录。我们推测CDGB或eve蛋白在基础启动子中占据第二个位点会抑制随后的TFIID结合,从而抑制转录,我们称之为协作阻断。

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