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恒定结构域调控抗体催化。

Constant domain-regulated antibody catalysis.

机构信息

Chemical Immunology Research Center, Department of Pathology and Laboratory Medicine, University of Texas Houston Medical School, Houston, Texas 77030, USA.

出版信息

J Biol Chem. 2012 Oct 19;287(43):36096-104. doi: 10.1074/jbc.M112.401075. Epub 2012 Sep 4.

Abstract

Some antibodies contain variable (V) domain catalytic sites. We report the superior amide and peptide bond-hydrolyzing activity of the same heavy and light chain V domains expressed in the IgM constant domain scaffold compared with the IgG scaffold. The superior catalytic activity of recombinant IgM was evident using two substrates, a small model peptide that is hydrolyzed without involvement of high affinity epitope binding, and HIV gp120, which is recognized specifically by noncovalent means prior to the hydrolytic reaction. The catalytic activity was inhibited by an electrophilic phosphonate diester, consistent with a nucleophilic catalytic mechanism. All 13 monoclonal IgMs tested displayed robust hydrolytic activities varying over a 91-fold range, consistent with expression of the catalytic functions at distinct levels by different V domains. The catalytic activity of polyclonal IgM was superior to polyclonal IgG from the same sera, indicating that on average IgMs express the catalytic function at levels greater than IgGs. The findings indicate a favorable effect of the remote IgM constant domain scaffold on the integrity of the V-domain catalytic site and provide a structural basis for conceiving antibody catalysis as a first line immune function expressed at high levels prior to development of mature IgG class antibodies.

摘要

一些抗体包含可变(V)结构域催化位点。我们报告了相同的重链和轻链 V 结构域在 IgM 恒定结构域支架中表达的优于 IgG 支架的酰胺和肽键水解活性。使用两种底物,一种小的模型肽,其水解不涉及高亲和力表位结合,以及 HIV gp120,在水解反应之前通过非共价方式特异性识别,重组 IgM 的优越催化活性是明显的。催化活性被亲电膦酸二酯抑制,与亲核催化机制一致。所有 13 种测试的单克隆 IgM 均显示出强大的水解活性,差异高达 91 倍,这与不同 V 结构域以不同水平表达催化功能一致。多克隆 IgM 的催化活性优于来自同一血清的多克隆 IgG,表明 IgM 平均以高于 IgG 的水平表达催化功能。这些发现表明远程 IgM 恒定结构域支架对 V 结构域催化位点的完整性有有利影响,并为设想抗体催化作为在成熟 IgG 类抗体产生之前以高水平表达的一线免疫功能提供了结构基础。

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