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绘制内质网相互作用组:钙连蛋白和钙网蛋白的P结构域作为折叠酶和伴侣蛋白的多价衔接子

Mapping the ER Interactome: The P Domains of Calnexin and Calreticulin as Plurivalent Adapters for Foldases and Chaperones.

作者信息

Kozlov Guennadi, Muñoz-Escobar Juliana, Castro Karla, Gehring Kalle

机构信息

Department of Biochemistry, Groupe de recherche axé sur la Structure des protéines, McGill University, 3649 Promenade Sir William Osler, Montréal, QC H3G 0B1, Canada.

Department of Biochemistry, Groupe de recherche axé sur la Structure des protéines, McGill University, 3649 Promenade Sir William Osler, Montréal, QC H3G 0B1, Canada.

出版信息

Structure. 2017 Sep 5;25(9):1415-1422.e3. doi: 10.1016/j.str.2017.07.010.

Abstract

The lectin chaperones calreticulin (CRT) and calnexin (CNX) contribute to the folding of glycoproteins in the ER by recruiting foldases such as the protein disulfide isomerase ERp57 and the peptidyl prolyl cis-trans isomerase CypB. Recently, CRT was shown to interact with the chaperone ERp29. Here, we show that ERp29 directly binds to the P domain of CNX. Crystal structures of the D domain of ERp29 in complex with the P domains from CRT and calmegin, a tissue-specific CNX homolog, reveal a commonality in the mechanism of binding whereby the tip of the P domain functions as a plurivalent adapter to bind a variety of folding factors. We show that mutation of a single residue, D348 in CNX, abrogates binding to ERp29 as well as ERp57 and CypB. The structural diversity of the accessory factors suggests that these chaperones became specialized for glycoprotein folding through convergent evolution of their P-domain binding sites.

摘要

凝集素伴侣钙网蛋白(CRT)和钙连蛋白(CNX)通过招募诸如蛋白二硫键异构酶ERp57和肽基脯氨酰顺反异构酶CypB等折叠酶,促进内质网中糖蛋白的折叠。最近研究表明,CRT可与伴侣蛋白ERp29相互作用。在此,我们发现ERp29可直接结合CNX的P结构域。ERp29的D结构域与CRT以及组织特异性CNX同源物钙调神经磷酸酶的P结构域形成复合物的晶体结构,揭示了结合机制的共性,即P结构域的末端作为多价衔接子,可结合多种折叠因子。我们发现,CNX中单个残基D348发生突变后,会消除其与ERp29以及ERp57和CypB的结合。辅助因子的结构多样性表明,这些伴侣蛋白通过其P结构域结合位点的趋同进化,专门用于糖蛋白折叠。

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