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Insights into E3 ligase activity revealed by a SUMO-RanGAP1-Ubc9-Nup358 complex

机译:SUMO-RanGAP1-Ubc9-Nup358复合体揭示的E3连接酶活性的见解

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SUMO-1 ( for small ubiquitin-related modifier) belongs to the ubiquitin (Ub) and ubiquitin-like (Ubl) protein family. SUMO conjugation occurs on specific lysine residues within protein targets, regulating pathways involved in differentiation, apoptosis, the cell cycle and responses to stress by altering protein function through changes in activity or cellular localization or by protecting substrates from ubiquitination(1,2). Ub/Ubl conjugation occurs in sequential steps and requires the concerted action of E2 conjugating proteins and E3 ligases(1,2). In addition to being a SUMO E3, the nucleoporin Nup358/RanBP2 localizes SUMO-conjugated RanGAP1 to the cytoplasmic face of the nuclear pore complex by means of interactions in a complex that also includes Ubc9, the SUMO E2 conjugating protein(3-6). Here we describe the 3.0-angstrom crystal structure of a four-protein complex of Ubc9, a Nup358/RanBP2 E3 ligase domain ( IR1-M) and SUMO-1 conjugated to the carboxy-terminal domain of RanGAP1. Structural insights, combined with biochemical and kinetic data obtained with additional substrates, support a model in which Nup358/ RanBP2 acts as an E3 by binding both SUMO and Ubc9 to position the SUMO - E2- thioester in an optimal orientation to enhance conjugation.
机译:SUMO-1(用于小的泛素相关修饰剂)属于泛素(Ub)和类泛素(Ubl)蛋白家族。 SUMO缀合发生在蛋白质靶标中的特定赖氨酸残基上,通过通过改变活性或细胞定位来改变蛋白质功能或通过保护底物免受泛素化来调节涉及分化,凋亡,细胞周期和应激反应的途径(1,2)。 Ub / Ubl偶联发生在顺序步骤中,需要E2偶联蛋白和E3连接酶的协同作用(1,2)。除了是SUMO E3外,核孔蛋白Nup358 / RanBP2还通过复合物中的相互作用将SUMO偶联的RanGAP1定位在核孔复合体的细胞质表面,该复合物还包含SUMO E2结合蛋白Ubc9(3-6)。在这里,我们描述了Ubc9,Nup358 / RanBP2 E3连接酶结构域(IR1-M)和SUMO-1与RanGAP1的羧基末端结构域共轭的四蛋白复合物的3.0埃晶体结构。结构的见解,结合使用其他底物获得的生化和动力学数据,支持了一种模型,其中Nup358 / RanBP2通过将SUMO和Ubc9结合以将SUMO-E2-硫酯定位在最佳方向上以增强缀合而充当E3。

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