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一种参与肠道相关免疫的人唾液蛋白的超抗原特性

Superantigen properties of a human sialoprotein involved in gut-associated immunity.

作者信息

Silverman G J, Roben P, Bouvet J P, Sasano M

机构信息

Sam and Rose Stein Institute for Research on Aging, University of California, San Diego, La Jolla 92093, USA.

出版信息

J Clin Invest. 1995 Jul;96(1):417-26. doi: 10.1172/JCI118051.

Abstract

Protein Fv (pFv) is a recently described 175-kD gut-associated sialoprotein with a potent capacity for augmentation of antibody-dependent immune functions. To investigate the molecular basis for Fab-mediated binding of pFv, we evaluated a panel of 52 monoclonal IgM and found that approximately 40% bound pFv. Whereas the majority (> or = 75%) of V H3 and V H6 IgM strongly bound pFv, only a small minority (< 20%) of IgM from other V H families bound pFv, and these antibodies had weaker binding interactions. Inhibition studies suggested that all binding occurred at the same (or overlapping) site(s) on pFv. Surface plasmon resonance studies demonstrated binding affinity constants up to 6.7 x 10(8) M-1 for pFv. Biopanning of IgM and IgG Fab phage-display libraries with pFv preferentially selected for V H3 and V H6 antibodies, but also obtained certain V H4 IgM. V H sequence analyses of 36 pFv-binding antibodies revealed that binding did not correlate with CDR sequence, JH, or L chain usage. However, there was preferential selection of pFv binders with V H CDR3 of small size. These studies demonstrate that a protein which enhances immune defense in the gut has structural and functional properties similar to known superantigens.

摘要

蛋白质Fv(pFv)是一种最近被描述的175kD的肠道相关唾液蛋白,具有增强抗体依赖性免疫功能的强大能力。为了研究Fab介导的pFv结合的分子基础,我们评估了一组52种单克隆IgM,发现约40%能结合pFv。虽然大多数(≥75%)的VH3和VH6 IgM能强烈结合pFv,但来自其他VH家族的IgM只有一小部分(<20%)能结合pFv,且这些抗体的结合相互作用较弱。抑制研究表明,所有结合都发生在pFv上相同(或重叠)的位点。表面等离子体共振研究表明,pFv的结合亲和力常数高达6.7×10⁸ M⁻¹。用pFv对IgM和IgG Fab噬菌体展示文库进行生物淘选,优先选择了VH3和VH6抗体,但也获得了某些VH4 IgM。对36种pFv结合抗体的VH序列分析表明,结合与CDR序列、JH或轻链使用情况无关。然而,优先选择了VH CDR3较小的pFv结合剂。这些研究表明,一种在肠道中增强免疫防御的蛋白质具有与已知超抗原相似的结构和功能特性。

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