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鉴定 RNA 结合蛋白低复杂度结构域老化液滴的刚性核心。

Identification of the Rigid Core for Aged Liquid Droplets of an RNA-Binding Protein Low Complexity Domain.

机构信息

Department of Chemistry, University of California, Davis, California 95616, United States.

出版信息

J Am Chem Soc. 2021 May 5;143(17):6657-6668. doi: 10.1021/jacs.1c02424. Epub 2021 Apr 25.

Abstract

The biomolecular condensation of proteins with low complexity sequences plays a functional role in RNA metabolism and a pathogenic role in neurodegenerative diseases. The formation of dynamic liquid droplets brings biomolecules together to achieve complex cellular functions. The rigidification of liquid droplets into β-strand-rich hydrogel structures composed of protein fibrils is thought to be purely pathological in nature. However, low complexity sequences often harbor multiple fibril-prone regions with delicately balanced functional and pathological interactions. Here, we investigate the maturation of liquid droplets formed by the low complexity domain of the TAR DNA-binding protein 43 (TDP-43). Solid state nuclear magnetic resonance measurements on the aged liquid droplets identify residues 365-400 as the structured core, which are squarely outside the region between residues 311-360 thought to be most important for pathological fibril formation and aggregation. The results of this study suggest that multiple segments of this low complexity domain are prone to form fibrils and that stabilization of β-strand-rich structure in one segment precludes the other region from adopting a rigid fibril structure.

摘要

低复杂度序列的蛋白质生物分子凝聚在 RNA 代谢中发挥功能作用,并在神经退行性疾病中发挥致病作用。动态液滴的形成将生物分子聚集在一起,以实现复杂的细胞功能。液滴的刚性化为由蛋白质原纤维组成的富含β-链的水凝胶结构被认为纯粹是病理性的。然而,低复杂度序列通常含有多个原纤维倾向区域,具有微妙平衡的功能和病理相互作用。在这里,我们研究了 TAR DNA 结合蛋白 43(TDP-43)的低复杂度结构域形成的液滴的成熟过程。对老化的液滴进行固态核磁共振测量,确定残基 365-400 为结构核心,这正好在被认为对病理性原纤维形成和聚集最重要的残基 311-360 之外。这项研究的结果表明,该低复杂度结构域的多个片段都容易形成原纤维,并且一个片段中富含β-链结构的稳定性阻止了另一个区域形成刚性原纤维结构。

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