泛素依赖性膜运输的分子机制。
Molecular mechanisms of ubiquitin-dependent membrane traffic.
机构信息
Laboratory of Molecular Biology, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892-0580, USA.
出版信息
Annu Rev Biophys. 2011;40:119-42. doi: 10.1146/annurev-biophys-042910-155404.
Abstract
Over the past 14 years, ubiquitination has emerged as a centrally important mechanism governing the subcellular trafficking of proteins. Ubiquitination, interaction with sorting factors that contain ubiquitin-binding domains, and deubiquitination govern the itineraries of cargo proteins that include yeast carboxypeptidase S, the epithelial sodium channel ENaC, and epidermal growth factor receptor. The molecular structures and mechanisms of the paradigmatic HECT and RING domain ubiquitin ligases, of JAMM- and USP-domain-deubiquitinating enzymes, and of numerous ubiquitin-binding domains involved in these pathways have been worked out in recent years and are described.
摘要
在过去的 14 年中,泛素化已成为控制蛋白质细胞内运输的一种重要机制。泛素化、与含有泛素结合域的分拣因子相互作用以及去泛素化决定了货物蛋白的行程,包括酵母羧肽酶 S、上皮钠离子通道 ENaC 和表皮生长因子受体。近年来,已经阐明了具有代表性的 HECT 和 RING 结构域泛素连接酶、JAMM 和 USP 结构域去泛素化酶以及涉及这些途径的众多泛素结合域的分子结构和机制,并进行了描述。
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