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白内障相关的 P23T γD-晶体蛋白在生理 pH 下形成的无定形外观聚集体中保留了类似天然的折叠结构。

Cataract-associated P23T γD-crystallin retains a native-like fold in amorphous-looking aggregates formed at physiological pH.

机构信息

Department of Structural Biology, University of Pittsburgh School of Medicine, 3501 Fifth Avenue, Pittsburgh, Pennsylvania 15213, USA.

The Center for Protein Conformational Diseases, University of Pittsburgh, Pittsburgh, Pennsylvania 15213, USA.

出版信息

Nat Commun. 2017 May 5;8:15137. doi: 10.1038/ncomms15137.

Abstract

Cataracts cause vision loss through the large-scale aggregation of eye lens proteins as a result of ageing or congenital mutations. The development of new treatments is hindered by uncertainty about the nature of the aggregates and their mechanism of formation. We describe the structure and morphology of aggregates formed by the P23T human γD-crystallin mutant associated with congenital cataracts. At physiological pH, the protein forms aggregates that look amorphous and disordered by electron microscopy, reminiscent of the reported formation of amorphous deposits by other crystallin mutants. Surprisingly, solid-state NMR reveals that these amorphous deposits have a high degree of structural homogeneity at the atomic level and that the aggregated protein retains a native-like conformation, with no evidence for large-scale misfolding. Non-physiological destabilizing conditions used in many in vitro aggregation studies are shown to yield qualitatively different, highly misfolded amyloid-like fibrils.

摘要

白内障会导致视力丧失,其原因是眼睛晶状体蛋白因衰老或先天突变而大规模聚集。由于对聚集物的性质及其形成机制的不确定性,新的治疗方法的发展受到了阻碍。我们描述了与先天性白内障有关的 P23T 人γD-晶体蛋白突变体形成的聚集体的结构和形态。在生理 pH 值下,该蛋白质形成的聚集体在电子显微镜下看起来无定形且无序,这让人联想到其他晶体蛋白突变体报告的无定形沉积物的形成。令人惊讶的是,固态 NMR 显示,这些无定形沉积物在原子水平上具有高度的结构均一性,并且聚集的蛋白质保留了类似天然的构象,没有大规模错误折叠的证据。在许多体外聚集研究中使用的非生理不稳定条件会产生定性不同的、高度错误折叠的类淀粉样纤维。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3fe/5424181/1ef68f1c08ea/ncomms15137-f1.jpg

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