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首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >A SUMO-dependent interaction between Senataxin and the exosome, disrupted in the neurodegenerative disease AOA2, targets the exosome to sites of transcription-induced DNA damage
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A SUMO-dependent interaction between Senataxin and the exosome, disrupted in the neurodegenerative disease AOA2, targets the exosome to sites of transcription-induced DNA damage

机译:Senataxin与外泌体之间的SUMO依赖相互作用在神经退行性疾病AOA2中被破坏,将外泌体靶向转录诱导的DNA损伤位点

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摘要

Senataxin (SETX) is an RNA/DNA helicase implicated in transcription termination and the DNA damage response and is mutated in two distinct neurological disorders: AOA2 (ataxia oculomotor apraxia 2) and ALS4 (amyotrophic lateral sclerosis 4). Here we provide evidence that Rrp45, a subunit of the exosome, associates with SETX in a manner dependent on SETX sumoylation.We show that the interaction and SETX sumoylation are disrupted by SETX mutations associated with AOA2 but not ALS4. Furthermore, Rrp45 colocalizes with SETX in distinct foci upon induction of transcription-related DNA damage. Our results thus provide evidence for a SUMO-dependent interaction between SETX and the exosome, disrupted in AOA2, that targets the exosome to sites of DNA damage.
机译:Senataxin(SETX)是一种RNA / DNA解旋酶,与转录终止和DNA损伤反应有关,并且在两种不同的神经系统疾病中发生突变:AOA2(共济失调性运动失用症2)和ALS4(肌萎缩性侧索硬化症4)。在这里,我们提供了证据,表明外泌体的一个亚基Rrp45与SETX的结合方式依赖于SETX sumoylation。我们表明相互作用和SETX sumoylation被与AOA2相关的SETX突变而不是与ALS4相关的突变所破坏。此外,在转录相关的DNA损伤诱导后,Rrp45与SETX在不同的焦点共定位。因此,我们的结果提供了SETX与外泌体之间的SUMO依赖性相互作用的证据,该相互作用在AOA2中受到破坏,从而将外泌体靶向DNA损伤位点。

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