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首页> 外文期刊>Journal of proteome research >Insights into the molecular composition of endogenous unanchored polyubiquitin chains
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Insights into the molecular composition of endogenous unanchored polyubiquitin chains

机译:洞察内源性非锚定多聚泛素链的分子组成

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The diverse influences of ubiquitin, mediated by its post-translational covalent modification of other proteins, have been extensively investigated. However, more recently roles for unanchored (nonsubstrate linked) polyubiquitin chains have also been proposed. Here we describe the use of ubiquitin-binding domains to affinity purify endogenous unanchored polyubiquitin chains and their subsequent characterization by mass spectrometry (MS). Using the A20 Znf domain of the ubiquitin receptor ZNF216 we isolated a protein from skeletal muscle shown by a combination of nanoLC-MS and LC-MS/MS to represent an unmodified and unanchored K48-linked ubiquitin dimer. Selective purification of unanchored polyubiquitin chains using the Znf UBP (BUZ) domain of USP5/isopeptidase-T allowed the isolation of K48 and K11-linked ubiquitin dimers, as well as revealing longer chains containing as many as 15 ubiquitin moieties, which include the K48 linkage. Top-down nanoLC-MS/MS of the A20 Znf-purified ubiquitin dimer generated diagnostic ions consistent with the presence of the K48 linkage, illustrating for the first time the potential of this approach to probe connectivity within endogenous polyubiquitin modifications. As well as providing initial proteomic insights into the molecular composition of endogenous unanchored polyubiquitin chains, this work also represents the first definition of polyubiquitin chain length in vivo.
机译:已经广泛研究了遍在蛋白由其他蛋白的翻译后共价修饰介导的各种影响。然而,最近也提出了非锚定的(非底物连接的)聚泛素链的作用。在这里,我们描述了使用泛素结合结构域亲和纯化内源未锚定的聚泛素链及其随后通过质谱(MS)表征的方法。使用泛素受体ZNF216的A20 Znf结构域,我们从骨骼肌中分离出一种蛋白质,该蛋白质通过nanoLC-MS和LC-MS / MS的组合显示,代表未修饰和未锚定的K48连接的泛素二聚体。使用USP5 /异肽酶-T的Znf UBP(BUZ)结构域选择性纯化未锚定的多聚泛素链,可以分离K48和K11连接的泛素二聚体,并揭示出包含多达15个泛素部分(包括K48)的更长链连锁。 A20 Znf纯化的泛素二聚体的自上而下的nanoLC-MS / MS产生与K48连锁存在一致的诊断离子,这首次证明了这种方法探测内源性多聚泛素修饰内连接性的潜力。除了提供对内源性非锚定多聚泛素链分子组成的蛋白质组学初步了解之外,这项工作还代表了体内多聚泛素链长的第一个定义。

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