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The inducible elongin A elongation activation domain: structure function and interaction with the elongin BC complex.

机译:诱导型延伸蛋白A延伸激活域:结构功能和与延伸蛋白BC复合物的相互作用。

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摘要

The elongin (SIII) complex strongly stimulates the rate of elongation by RNA polymerase II by suppressing transient pausing by polymerase at many sites along the DNA. Elongin (SIII) is composed of a transcriptionally active A subunit and two small regulatory B and C subunits, which bind stably to each other to form a binary complex that interacts with elongin A and strongly induces its transcriptional activity. The elongin (SIII) complex is a potential target for negative regulation by the von Hippel-Lindau (VHL) tumor suppressor protein, which is capable of binding stably to the elongin BC complex and preventing it from activating elongin A. Here, we identify an elongin A domain sufficient for activation of elongation and demonstrate that it is a novel type of inducible activator that targets the RNA polymerase II elongation complex and is evolutionarily conserved in species as distantly related as Caenorhabditis elegans and man. In addition, we demonstrate that both the elongin A elongation activation domain and the VHL tumor suppressor protein interact with the elongin BC complex through a conserved elongin BC binding site motif that is essential for induction of elongin A activity by elongin BC and for tumor suppression by the VHL protein.
机译:延伸蛋白(SIII)复合物通过抑制DNA沿许多位点的聚合酶引起的瞬时停顿,强烈刺激了RNA聚合酶II的延伸速率。 Elongin(SIII)由转录活性A亚基和两个小的调节性B和C亚基组成,它们稳定地相互结合形成与Elongin A相互作用并强烈诱导其转录活性的二元复合物。延伸蛋白(SIII)复合物是von Hippel-Lindau(VHL)肿瘤抑制蛋白负调控的潜在目标,该蛋白能够稳定地与延伸蛋白BC复合物结合并阻止其激活延伸蛋白A。在这里,我们确定了延伸蛋白(elongin)一个足以激活延伸的结构域,证明它是靶向RNA聚合酶II延伸复合物的新型诱导型激活剂,在与秀丽隐杆线虫和人类有密切关系的物种中进化上保守。此外,我们证明,延伸蛋白A延伸激活域和VHL肿瘤抑制蛋白均通过保守的延伸蛋白BC结合位点基序与延伸蛋白BC复合物相互作用,这对于通过延伸蛋白BC诱导延伸蛋白A活性和通过抑制肿瘤抑制蛋白是必不可少的。 VHL蛋白。

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