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E2-25K泛素结合酶介导的多聚泛素环化作用。

Cyclization of polyubiquitin by the E2-25K ubiquitin conjugating enzyme.

作者信息

Yao T, Cohen R E

机构信息

Department of Biochemistry, University of Iowa, Iowa City, Iowa 52242, USA.

出版信息

J Biol Chem. 2000 Nov 24;275(47):36862-8. doi: 10.1074/jbc.M006050200.

DOI:10.1074/jbc.M006050200
PMID:10906148
Abstract

For most substrates of ubiquitin (Ub)-dependent degradation, recognition by the proteasome is mediated by a covalently attached signal assembled from multiple ubiquitins linked to each other via the C terminus of one Ub and the epsilon-amine of Lys(48) of another Ub. Among Ub-conjugating enzymes, E2-25K is unique in its ability to synthesize in vitro unanchored Lys(48)-linked poly-Ub chains from mono- or poly-Ub, E1, and ATP; thus, E2-25K has distinct binding sites for donor and acceptor (poly)Ub. During studies of chain assembly by E2-25K, we observed that Lys(48)-linked tri-Ub was efficiently converted to a new species that upon SDS-polyacrylamide gel electrophoresis migrated between linear di-Ub and tri-Ub. Analysis of this product by mass spectrometry and tryptic digestion showed that it was a cyclic form of tri-Ub. Cyclization of tri-Ub requires E1, E2-25K, ATP, and that the linear substrate has a free Gly(76) C terminus on the proximal end Ub and a Lys(48) side chain available on the distal end Ub. E2-25K similarly can catalyze the cyclization of longer poly-Ub chains, including tetra- and penta-Ub. Although cyclic tri-Ub resists hydrolysis by the PA700 or isopeptidase T deubiquitinating enzymes, it can be disassembled to Ub monomers by isopeptidase(s) in a red blood cell extract. Thus, if cyclic poly-Ub forms in vivo, it will not accumulate as a dead-end product.

摘要

对于大多数依赖泛素(Ub)的降解底物而言,蛋白酶体的识别是由一个共价连接的信号介导的,该信号由多个泛素组装而成,这些泛素通过一个泛素的C末端与另一个泛素的赖氨酸(Lys)48的ε-氨基相互连接。在泛素缀合酶中,E2-25K具有独特的能力,能够在体外从单泛素或多泛素、E1和ATP合成无锚定的赖氨酸(Lys)48连接的多聚泛素链;因此,E2-25K对供体和受体(多聚)泛素有不同的结合位点。在对E2-25K进行链组装的研究过程中,我们观察到赖氨酸(Lys)48连接的三泛素被有效地转化为一种新的物种,在十二烷基硫酸钠-聚丙烯酰胺凝胶电泳(SDS-聚丙烯酰胺凝胶电泳)中,其迁移位置介于线性二泛素和三泛素之间。通过质谱分析和胰蛋白酶消化对该产物进行分析表明,它是三泛素的环状形式。三泛素的环化需要E1、E2-25K、ATP,并且线性底物在近端泛素上有一个游离的甘氨酸(Gly)76 C末端,在远端泛素上有一个可用的赖氨酸(Lys)48侧链。E2-25K同样可以催化更长的多聚泛素链的环化,包括四泛素和五泛素。尽管环状三泛素可抵抗PA700或异肽酶T去泛素化酶的水解,但它可以在红细胞提取物中被异肽酶分解为泛素单体。因此,如果环状多聚泛素在体内形成,它不会作为终产物积累。

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