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多聚体组装的后生动物 AAA 伴侣蛋白将底物提取与重折叠偶联。

Dodecamer assembly of a metazoan AAA chaperone couples substrate extraction to refolding.

机构信息

Division of Chemistry and Chemical Engineering, California Institute of Technology, Pasadena, CA 91125, USA.

Department of Biochemistry and Biophysics, University of California at San Francisco, San Francisco, CA 94158, USA.

出版信息

Sci Adv. 2023 May 10;9(19):eadf5336. doi: 10.1126/sciadv.adf5336.

Abstract

Ring-forming AAA chaperones solubilize protein aggregates and protect organisms from proteostatic stress. In metazoans, the AAA chaperone Skd3 in the mitochondrial intermembrane space (IMS) is critical for human health and efficiently refolds aggregated proteins, but its underlying mechanism is poorly understood. Here, we show that Skd3 harbors both disaggregase and protein refolding activities enabled by distinct assembly states. High-resolution structures of Skd3 hexamers in distinct conformations capture ratchet-like motions that mediate substrate extraction. Unlike previously described disaggregases, Skd3 hexamers further assemble into dodecameric cages in which solubilized substrate proteins can attain near-native states. Skd3 mutants defective in dodecamer assembly retain disaggregase activity but are impaired in client refolding, linking the disaggregase and refolding activities to the hexameric and dodecameric states of Skd3, respectively. We suggest that Skd3 is a combined disaggregase and foldase, and this property is particularly suited to meet the complex proteostatic demands in the mitochondrial IMS.

摘要

成环 AAA 伴侣可溶解蛋白质聚集体并保护生物体免受蛋白质稳态应激。在后生动物中,线粒体间室(IMS)中的 AAA 伴侣 Skd3 对人类健康至关重要,可有效重折叠聚集的蛋白质,但它的潜在机制尚不清楚。在这里,我们表明 Skd3 具有两种解聚酶和蛋白质重折叠活性,这是由不同的组装状态实现的。Skd3 六聚体在不同构象中的高分辨率结构捕获了介导底物提取的棘轮样运动。与以前描述的解聚酶不同,Skd3 六聚体进一步组装成十二聚体笼,其中溶解的底物蛋白可以达到近天然状态。Skd3 突变体在十二聚体组装中缺陷,但在客户蛋白重折叠中受损,将解聚酶和重折叠活性分别与 Skd3 的六聚体和十二聚体状态联系起来。我们认为 Skd3 是一种组合的解聚酶和折叠酶,这种特性特别适合满足线粒体 IMS 中复杂的蛋白质稳态需求。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/64c4/10171807/0d0b63b49865/sciadv.adf5336-f1.jpg

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