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Reversible ADP-ribosylation of RNA

机译:RNA的可逆ADP-核糖基化

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摘要

ADP-ribosylation is a reversible chemical modification catalysed by ADP-ribosyltransferases such as PARPs that utilize nicotinamide adenine dinucleotide (NAD+) as a cofactor to transfer monomer or polymers of ADP-ribose nucleotide onto macromolecular targets such as proteins and DNA. ADP-ribosylation plays an important role in several biological processes such as DNA repair, transcription, chromatin remodelling, host-virus interactions, cellular stress response and many more. Using biochemical methods we identify RNA as a novel target of reversible mono-ADP-ribosylation. We demonstrate that the human PARPs - PARP10, PARP11 and PARP15 as well as a highly diverged PARP homologue TRPT1, ADP-ribosylate phosphorylated ends of RNA. We further reveal that ADP-ribosylation of RNA mediated by PARP10 and TRPT1 can be efficiently reversed by several cellular ADP-ribosylhydrolases (PARG, TARG1, MACROD1, MACROD2 and ARH3), as well as by MACROD-like hydrolases from VEEV and SARS viruses. Finally, we show that TRPT1 and MACROD homologues in bacteria possess activities equivalent to the human proteins. Our data suggest that RNA ADP-ribosylation may represent a widespread and physiologically relevant form of reversible ADP-ribosylation signalling.
机译:ADP-核糖基化是由ADP-核糖基转移酶(如PARPs)催化的可逆化学修饰,其利用烟酰胺腺嘌呤二核苷酸(NAD + )作为辅因子将ADP-核糖核苷酸的单体或聚合物转移至大分子靶标上,例如蛋白质和DNA。 ADP-核糖基化在几个生物学过程中起着重要作用,例如DNA修复,转录,染色质重塑,宿主-病毒相互作用,细胞应激反应等。使用生化方法,我们确定RNA为可逆的单ADP核糖基化的新目标。我们证明了人类PARPs-PARP10,PARP11和PARP15以及高度分散的PARP同源物TRPT1,RNA的ADP-核糖基磷酸化末端。我们进一步揭示了由PARP10和TRPT1介导的RNA的ADP-核糖基化可以被几种细胞ADP-核糖基水解酶(PARG,TARG1,MACROD1,MACROD2和ARH3)以及VEEV和SARS病毒的MACROD样水解酶有效逆转。最后,我们显示细菌中的TRPT1和MACROD同源物具有与人类蛋白质相同的活性。我们的数据表明,RNA ADP-核糖基化可能代表了可逆性ADP-核糖基化信号的广泛且生理相关的形式。

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