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人血浆来源的多聚免疫球蛋白 A 和免疫球蛋白 M 抗体与分泌成分结合,产生具有生物活性的分泌样抗体。

Human plasma-derived polymeric IgA and IgM antibodies associate with secretory component to yield biologically active secretory-like antibodies.

机构信息

R&D Laboratory of the Division of Immunology and Allergy, Centre Hospitalier Universitaire Vaudois, Rue du Bugnon, 1011 Lausanne, Switzerland.

出版信息

J Biol Chem. 2013 Feb 8;288(6):4085-94. doi: 10.1074/jbc.M112.410811. Epub 2012 Dec 18.

Abstract

Immunotherapy with monoclonal and polyclonal immunoglobulin is successfully applied to improve many clinical conditions, including infection, autoimmune diseases, or immunodeficiency. Most immunoglobulin products, recombinant or plasma-derived, are based on IgG antibodies, whereas to date, the use of IgA for therapeutic application has remained anecdotal. In particular, purification or production of large quantities of secretory IgA (SIgA) for potential mucosal application has not been achieved. In this work, we sought to investigate whether polymeric IgA (pIgA) recovered from human plasma is able to associate with secretory component (SC) to generate SIgA-like molecules. We found that ∼15% of plasma pIgA carried J chain and displayed selective SC binding capacity either in a mixture with monomeric IgA (mIgA) or after purification. The recombinant SC associated covalently in a 1:1 stoichiometry with pIgA and with similar efficacy as colostrum-derived SC. In comparison with pIgA, the association with SC delayed degradation of SIgA by intestinal proteases. Similar results were obtained with plasma-derived IgM. In vitro, plasma-derived IgA and SIgA neutralized Shigella flexneri used as a model pathogen, resulting in a delay of bacteria-induced damage targeted to polarized Caco-2 cell monolayers. The sum of these novel data demonstrates that association of plasma-derived IgA or IgM with recombinant/colostrum-derived SC is feasible and yields SIgA- and SIgM-like molecules with similar biochemical and functional characteristics as mucosa-derived immunoglobulins.

摘要

免疫球蛋白的单克隆和多克隆免疫疗法已成功应用于改善许多临床状况,包括感染、自身免疫性疾病或免疫缺陷。大多数免疫球蛋白产品,无论是重组的还是血浆衍生的,都是基于 IgG 抗体,而迄今为止,IgA 用于治疗应用的情况仍只是传闻。特别是,尚未实现用于潜在黏膜应用的大量分泌型 IgA(SIgA)的纯化或生产。在这项工作中,我们试图研究从人血浆中回收的多聚 IgA(pIgA)是否能够与分泌成分(SC)结合以产生 SIgA 样分子。我们发现,约 15%的血浆 pIgA 携带 J 链,并显示出选择性的 SC 结合能力,无论是在与单体 IgA(mIgA)的混合物中还是在纯化后。重组 SC 以 1:1 的化学计量比与 pIgA 共价结合,与初乳衍生的 SC 具有相似的功效。与 pIgA 相比,SC 的结合延迟了肠道蛋白酶对 SIgA 的降解。用血浆衍生的 IgM 进行的比较也得到了类似的结果。在体外,血浆衍生的 IgA 和 SIgA 中和了用作模型病原体的福氏志贺菌,导致针对极化 Caco-2 细胞单层的细菌诱导损伤的延迟。这些新数据表明,将血浆衍生的 IgA 或 IgM 与重组/初乳衍生的 SC 结合是可行的,并且产生的 SIgA 和 SIgM 样分子具有与黏膜衍生的免疫球蛋白相似的生化和功能特征。

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