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Structure-Function Analysis of the Human TFIIB-Related Factor II Protein Reveals an Essential Role for the C-Terminal Domain in RNA Polymerase III Transcription

机译:人TFIIB相关因子II蛋白的结构功能分析揭示了RNA聚合酶III转录中C末端域的基本作用。

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The transcription factors TFIIB, Brf1, and Brf2 share related N-terminal zinc ribbon and core domains. TFIIB bridges RNA polymerase II (Pol II) with the promoter-bound preinitiation complex, whereas Brf1 and Brf2 are involved, as part of activities also containing TBP and Bdp1 and referred to here as Brf1-TFIIIB and Brf2-TFIIIB, in the recruitment of Pol III. Brf1-TFIIIB recruits Pol III to type 1 and 2 promoters and Brf2-TFIIIB to type 3 promoters such as the human U6 promoter. Brf1 and Brf2 both have a C-terminal extension absent in TFIIB, but their C-terminal extensions are unrelated. In yeast Brf1, the C-terminal extension interacts with the TBP/TATA box complex and contributes to the recruitment of Bdp1. Here we have tested truncated Brf2, as well as Brf2/TFIIB chimeric proteins for U6 transcription and for assembly of U6 preinitiation complexes. Our results characterize functions of various human Brf2 domains and reveal that the C-terminal domain is required for efficient association of the protein with U6 promoter-bound TBP and SNAPc, a type 3 promoter-specific transcription factor, and for efficient recruitment of Bdp1. This in turn suggests that the C-terminal extensions in Brf1 and Brf2 are crucial to specific recruitment of Pol III over Pol II.
机译:转录因子TFIIB,Brf1和Brf2共享相关的N末端锌带和核心结构域。 TFIIB通过启动子结合的预起始复合物桥接RNA聚合酶II(Pol II),而在参与招募的过程中,Brf1和Brf2作为也包含TBP和Bdp1的活动的一部分参与,在本文中也称为Brf1-TFIIIB和Brf2-TFIIIB。波尔三。 Brf1-TFIIIB将Pol III募集为1型和2型启动子,Brf2-TFIIIB募集为3型启动子,例如人U6启动子。 Brf1和Brf2都在TFIIB中不存在C末端延伸,但是它们的C末端延伸无关。在酵母Brf1中,C末端延伸与TBP / TATA盒复合体相互作用,并有助于Bdp1的募集。在这里,我们已经测试了截短的Brf2以及Brf2 / TFIIB嵌合蛋白,用于U6转录和U6预启动复合物的组装。我们的结果表征了各种人类Brf2域的功能,并揭示了C末端域是蛋白质与U6启动子结合的TBP和SNAP c (3型启动子特异性转录因子)有效结合所必需的,并有效招募Bdp1。这反过来表明Brf1和Brf2的C末端延伸对于Pol II特异于Pol II的募集至关重要。

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