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Poly(ADP-ribose) regulates post-transcriptional gene regulation in the cytoplasm

机译:聚(ADP-核糖)调节细胞质中的转录后基因调控

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Since its discovery in 1963, poly(ADP-ribose) (pADPr) has been shown to play important functions in the nucleus of multicellular eukaryotes. Each of these functions centers upon DNA metabolism, including DNA-damage repair, chromatin remodeling, transcription and telomere functions. We recently described two novel functions for pADPr in the cytoplasm, both of which involve RNA metabolism - (1) the assembly of cytoplasmic stress granules, cellular macrostructures that aggregate translationally stalled mRNA/protein complexes and (2) modulation of microRNA activities. Multiple stress granule-localized, post-transcriptional gene regulators, including microRNA-binding argonaute family members, are substrates for pADPr modification and are increasingly modified by pADPr upon stress. Interestingly, the cytoplasmic RNA regulatory functions for PARPs are likely mediated through activities of catalytically inactive PARP-13/ARTD13/ZC3HAV1/ZAP and mono/poly(ADP-ribose)-synthesizing enzymes, including PARP-5a/ARTD5/TNKS1, PARP-12/ARTD12/ZC3HDC1 and PARP-15/ARTD7/BAL3. These data are consistent with other recent work, which suggests that mono(ADP-ribosyl)ated residues can be poly(ADP-ribosyl)ated by different enzymes.
机译:自1963年发现以来,聚(ADP-核糖)(pADPr)已显示在多细胞真核生物的核中起重要作用。这些功能均以DNA代谢为中心,包括DNA损伤修复,染色质重塑,转录和端粒功能。我们最近描述了pADPr在细胞质中的两个新功能,均涉及RNA代谢-(1)细胞质应激颗粒的组装,聚集翻译停滞的mRNA /蛋白质复合物的细胞宏观结构和(2)microRNA活性的调节。多种应激颗粒定位的转录后基因调节剂,包括与microRNA结合的argonaute家族成员,是pADPr修饰的底物,并在压力下被pADPr修饰。有趣的是,PARP的胞质RNA调节功能可能是通过催化失活的PARP-13 / ARTD13 / ZC3HAV1 / ZAP和单/聚(ADP-核糖)合成酶(包括PARP-5a / ARTD5 / TNKS1,PARP- 12 / ARTD12 / ZC3HDC1和PARP-15 / ARTD7 / BAL3。这些数据与其他最近的工作一致,这表明单(ADP-核糖基)化的残基可以被不同的酶聚(ADP-核糖基)化。

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