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解析内质网中无规则卷曲 Ca2+缓冲伴侣钙网蛋白的物理结构。

Dissecting physical structure of calreticulin, an intrinsically disordered Ca-buffering chaperone from endoplasmic reticulum.

机构信息

a Tisch Cancer Institute, Icahn School of Medicine at Mount Sinai (ISMMS) , New York , NY , USA.

b Department of Biomedical and Neuromotorial Sciences , Alma Mater University , Bologna , Italy.

出版信息

J Biomol Struct Dyn. 2018 May;36(6):1617-1636. doi: 10.1080/07391102.2017.1330224. Epub 2017 May 26.

Abstract

Calreticulin (CALR) is a Ca binding multifunctional protein that mostly resides in the endoplasmic reticulum (ER) and plays a number of important roles in various physiological and pathological processes. Although the major functions ascribed to CALR are controlling the Ca homeostasis in ER and acting as a lectin-like ER chaperon for many glycoproteins, this moonlighting protein can be found in various cellular compartments where it has many non-ER functions. To shed more light on the mechanisms underlying polyfunctionality of this moonlighting protein that can be found in different cellular compartments and that possesses a wide spectrum of unrelated biological activities, being able to interact with Ca (and potentially other metal ions), RNA, oligosaccharides, and numerous proteins, we used a set of experimental and computational tools to evaluate the intrinsic disorder status of CALR and the role of calcium binding on structural properties and conformational stability of the full-length CALR and its isolated P- and C-domains.

摘要

钙网蛋白(CALR)是一种 Ca 结合多功能蛋白,主要位于内质网(ER)中,在各种生理和病理过程中发挥着许多重要作用。尽管钙网蛋白的主要功能是控制 ER 中的 Ca 稳态,并作为许多糖蛋白的凝集素样 ER 伴侣,但这种兼职蛋白可以在各种细胞区室中找到,在那里它具有许多非 ER 功能。为了更深入地了解这种兼职蛋白在不同细胞区室中的多功能性的机制,这种兼职蛋白具有广泛的无关生物活性,能够与 Ca(和潜在的其他金属离子)、RNA、寡糖和许多蛋白质相互作用,我们使用了一组实验和计算工具来评估 CALR 的固有无序状态以及钙结合对全长 CALR 及其分离的 P 域和 C 域的结构特性和构象稳定性的作用。

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