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Structure and function of Parkin E3 ubiquitin ligase reveals aspects of RING and HECT ligases

机译:Parkin E3泛素连接酶的结构和功能揭示了RING和HECT连接酶的各个方面

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摘要

Parkin is a RING-between-RING E3 ligase that functions in the covalent attachment of ubiquitin to specific substrates, and mutations in Parkin are linked to Parkinson’s disease, cancer and mycobacterial infection. The RING-between-RING family of E3 ligases are suggested to function with a canonical RING domain and a catalytic cysteine residue usually restricted to HECT E3 ligases, thus termed ‘RING/HECT hybrid’ enzymes. Here we present the 1.58 Å structure of Parkin-R0RBR, revealing the fold architecture for the four RING domains, and several unpredicted interfaces. Examination of the Parkin active site suggests a catalytic network consisting of C431 and H433. In cells, mutation of C431 eliminates Parkin-catalysed degradation of mitochondria, and capture of an ubiquitin oxyester confirms C431 as Parkin’s cellular active site. Our data confirm that Parkin is a RING/HECT hybrid, and provide the first crystal structure of an RING-between-RING E3 ligase at atomic resolution, providing insight into this disease-related protein.
机译:帕金蛋白是一种介于RING与RING之间的RING连接酶,可在泛素与特定底物的共价结合中发挥作用,并且帕金森的突变与帕金森氏病,癌症和分枝杆菌感染有关。 E3连接酶的RING之间的RING家族建议与典型的RING域和通常限于HECT E3连接酶的催化半胱氨酸残基一起起作用,因此被称为“ RING / HECT hybrid”酶。在这里,我们介绍了Parkin-R0RBR的1.58Å结构,揭示了四个RING域的折叠结构以及一些不可预测的界面。对Parkin活性位点的检查表明存在一个由C431和H433组成的催化网络。在细胞中,C431的突变消除了Parkin催化的线粒体降解,捕获泛素含氧酸酯证实C431是Parkin的细胞活性位点。我们的数据证实,Parkin是RING / HECT杂种,并以原子分辨率提供RING-RING-E3连接酶的第一个晶体结构,从而提供了对该疾病相关蛋白的洞察力。

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