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The multi-tasking P-TEFb complex.

机译:多任务P-TEFb复合体。

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摘要

P-TEFb (CycT1:Cdk9), the metazoan RNA polymerase II Ser2 C-terminal domain (CTD) kinase, regulates transcription elongation at many genes and integrates mRNA synthesis with histone modification, pre-mRNA processing, and mRNA export. Recruitment of P-TEFb to target genes requires deubiquitination of H2Bub, phosphorylation of H3S10, and the bromodomain protein, Brd4. Brd4 activates growth-related genes in the G1 phase of the cell cycle and can also tether P-TEFb to mitotic chromosomes, possibly to mark sites of active transcription throughout cell division. P-TEFb co-operates with c-Myc during transactivation and cell transformation, and also requires SKIP (c-Ski-interacting protein), an mRNA elongation and splicing factor. Some functions of the P-TEFb/Ser2P CTD are executed by the Spt6 transcription elongation factor, which binds directly to the phosphorylated CTD and recruits the Iws1 ('interacts with Spt6') protein. Iws1, in turn, interacts with the REF1/Aly nuclear export adaptor and stimulates the kinetics of mRNA export. Given the prominent role of Spt6 in regulating chromatin structure, the CTD-bound Spt6:Iws1 complex may also control histone modifications during elongation. Following transcription, P-TEFb accompanies the mature mRNA to the cytoplasm to promote translation elongation.
机译:P-TEFb(CycT1:Cdk9),后生动物RNA聚合酶II Ser2 C末端域(CTD)激酶,调节许多基因的转录延伸,并将mRNA合成与组蛋白修饰,mRNA前加工和mRNA输出整合在一起。向目标基因招募P-TEFb需要H2Bub的去泛素化,H3S10的磷酸化和溴结构域蛋白Brd4。 Brd4在细胞周期的G1期激活与生长相关的基因,还可以将P-TEFb束缚在有丝分裂染色体上,可能标记整个细胞分裂过程中活跃转录的位点。 P-TEFb在反式激活和细胞转化过程中与c-Myc合作,还需要SKIP(与c-Ski相互作用的蛋白质),一种mRNA的延伸和剪接因子。 P-TEFb / Ser2P CTD的某些功能由Spt6转录延伸因子执行,该因子直接与磷酸化的CTD结合并募集Iws1(“与Spt6相互作用”)蛋白。 Iws1反过来与REF1 / Aly核输出衔接子相互作用,并刺激mRNA输出的动力学。鉴于Spt6在调节染色质结构中的重要作用,CTD结合的Spt6:Iws1复合物也可能在延伸过程中控制组蛋白修饰。转录后,P-TEFb将成熟的mRNA伴随到细胞质中以促进翻译延伸。

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