首页> 外文期刊>Current topics in microbiology and immunology >Regulation of Nucleocytoplasmk Transport by ADP-Ribosylation: The Emerging Role of Karyopherin-beta1 Mono-ADP-Ribosylation by ARTD15
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Regulation of Nucleocytoplasmk Transport by ADP-Ribosylation: The Emerging Role of Karyopherin-beta1 Mono-ADP-Ribosylation by ARTD15

机译:ADP-核糖基化的核细胞粒子k核酸输送的调节:浅谈浅谈核桃蛋白-ADP-核糖化的新兴作用

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Post-translational modifications of a cellular protein by mono- and poly-ADP-ribosylation involve the cleavage of NAD+, with the release of its nicotin-amide moiety. This is accompanied by the transfer of a single (mono-) or several (poly-) ADP-ribose molecules from NAD+ to a specific amino-acid residue of the protein. Recent reports have shed new light on the correlation between NAD -dependent ADP-ribosylation reactions and the endoplasmic reticulum, in addition lo the well-documented roles of these reactions in the nucleus and mitochondria. We have demonstrated that ARTD15/PARP16 is a novel mono-ADP-ribosyltransferase with a new intracellular location, as it is associated with the endoplasmic reticulum. The endoplasmic reticulum, which is a membranous network of interconnected tubules and cisternae, is responsible for specialised cellular functions, including protein folding and protein transport. Maintenance of specialised cellular functions requires the correct flow of information between separate organelles that is made possible through the nucleocytoplasmk trafficking of proteins. ARTD15 appears to have a role in nucleocytoplasmic shuttling, through karyopherin-betal mono-ADP-ribosylation. This is in line with the emerging role of ADP-ribosylation in the regulation of intracellular trafficking of cellular proteins. Indeed, other ,ADP-ribosyltransferases like ARTD1/PARP1, have been reported to regulate nucleocytoplasmic trafficking of crucial proteins, including p53 and NF-/cB, and as a consequence, to modulate the subcellular localisation of these proteins under both physiological and pathological conditions.
机译:通过单甘氨酸酰胺部分的释放,通过单 - 和聚-ADP-核糖化的翻译后修饰涉及NAD +的切割。这伴随着从NAD +转移单个(单型)或几种(多元)ADP-核糖分子到蛋白质的特定氨基酸残基。最近的报告揭示了NAD - 依赖性ADP-核糖基化反应与内质网之间的相关性,并且在细胞核和线粒体中这些反应的良好记录作用。我们已经证明,ArtD15 / PARP16是一种新型单adp-核糖基转移酶,其具有新的细胞内位置,因为它与内质网相关。作为相互连接的小管和闭合的膜网的内质网是负责专业的细胞功能,包括蛋白质折叠和蛋白质转运。通过通过蛋白质的核细胞立体贩运使得可以正确地进行专用蜂窝功能的维护需要正确的信息流动。 ARTD15似乎在核细胞质穿梭中具有作用,通过Karyopherin-Betal单-Ado-Adp-核糖化。这符合ADP-核糖基化在调节细胞蛋白的调节中的新兴作用。实际上,据报道,其他,ADP-罗基糖基转移酶如ARTD1 / PARP1,以调节关键蛋白质的核细胞质贩运,包括P53和NF-/ Cb,因此在生理和病理条件下调节这些蛋白质的亚细胞定位。

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