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Defining the Human Deubiquitinating Enzyme Interaction Landscape

机译:定义人类去泛素化酶相互作用的格局

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Deubiquitinating enzymes (Dubs) function to remove covalently attached ubiquitin from proteins, thereby controlling substrate activity and/or abundance. For most Dubs, their functions, targets, and regulation are poorly understood. To systematically investigate Dub function, we initiated a global proteomic analysis of Dubs and their associated protein complexes. This was accomplished through the development of a software platform called CompPASS, which uses unbiased metrics to assign confidence measurements to interactions from parallel nonreciprocal proteomic data sets. We identified 774 candidate interacting proteins associated with 75 Dubs. Using Gene Ontology, interactome topology classification, subcellular localization, and functional studies, we link Dubs to diverse processes, including protein turnover, transcription, RNA processing, DNA damage, and endoplasmic reticulum-associated degradation. This work provides the first glimpse into the Dub interaction landscape, places previously unstudied Dubs within putative biological pathways, and identifies previously unknown interactions and protein complexes involved in this increasingly important arm of the ubiquitin-proteasome pathway.
机译:去泛素化酶(Dubs)的功能是从蛋白质上去除共价连接的泛素,从而控制底物活性和/或丰度。对于大多数配音,他们的功能,目标和法规了解得很少。为了系统地研究Dub的功能,我们启动了Dubs及其相关蛋白复合物的全球蛋白质组学分析。这是通过开发一个名为CompPASS的软件平台来完成的,该平台使用无偏度量来将置信度度量值分配给来自并行非对等蛋白质组数据集的交互。我们确定了774个与75个Dub相关的候选相互作用蛋白。使用基因本体论,相互作用组拓扑分类,亚细胞定位和功能研究,我们将Dubs连接到各种过程,包括蛋白质更新,转录,RNA处理,DNA损伤和内质网相关的降解。这项工作提供了对Dub相互作用前景的初步了解,将先前未研究的Dub置于推定的生物途径中,并鉴定了在遍在蛋白-蛋白酶体途径这一日益重要的分支中涉及的先前未知的相互作用和蛋白质复合物。

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