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CH1结构域中的半胱氨酸是未组装的免疫球蛋白重链滞留的基础。

Cysteines in CH1 underlie retention of unassembled Ig heavy chains.

作者信息

Elkabetz Yechiel, Argon Yair, Bar-Nun Shoshana

机构信息

Department of Biochemistry, George S. Wise Faculty of Life Sciences, Tel Aviv University, Ramat Aviv, Tel Aviv 69978, Israel.

出版信息

J Biol Chem. 2005 Apr 15;280(15):14402-12. doi: 10.1074/jbc.M500161200. Epub 2005 Feb 10.

Abstract

Conformation, structure, and oligomeric state of immunoglobulins not only control quality and functional properties of antibodies but are also critical for immunoglobulins secretion. Unassembled immunoglobulin heavy chains are retained intracellularly by delayed folding of the C(H)1 domain and irreversible interaction of BiP with this domain. Here we show that the three C(H)1 cysteines play a central role in immunoglobulin folding, assembly, and secretion. Remarkably, ablating all three C(H)1 cysteines negates retention and enables BiP cycling and non-canonical folding and assembly. This phenomenon is explained by interdependent formation of intradomain and interchain disulfides, although both bonds are dispensable for secretion. Substituting Cys-195 prevents formation not only of the intradomain disulfide, but also of the interchain disulfide bond with light chain, BiP displacement, and secretion. Mutating the light chain-interacting Cys-128 hinders disulfide bonding of intradomain cysteines, allowing their opportunistic bonding with light chain, without hampering secretion. We propose that the role of C(H)1 cysteines in immunoglobulin assembly and secretion is not simply to engage in disulfide bridges, but to direct proper folding and interact with the retention machinery.

摘要

免疫球蛋白的构象、结构和寡聚状态不仅控制抗体的质量和功能特性,对免疫球蛋白的分泌也至关重要。未组装的免疫球蛋白重链通过C(H)1结构域的延迟折叠以及BiP与该结构域的不可逆相互作用而保留在细胞内。在此我们表明,三个C(H)1半胱氨酸在免疫球蛋白的折叠、组装和分泌中起核心作用。值得注意的是,去除所有三个C(H)1半胱氨酸可消除滞留现象,并使BiP循环以及非经典折叠和组装成为可能。尽管这两种键对于分泌并非必需,但这种现象可通过结构域内和链间二硫键的相互依赖形成来解释。取代Cys-195不仅会阻止结构域内二硫键的形成,还会阻止与轻链的链间二硫键形成、BiP置换和分泌。突变与轻链相互作用的Cys-128会阻碍结构域内半胱氨酸的二硫键结合,使其能够与轻链随机结合,而不会妨碍分泌。我们提出,C(H)1半胱氨酸在免疫球蛋白组装和分泌中的作用不仅仅是参与二硫键的形成,还在于指导正确折叠并与滞留机制相互作用。

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