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抗体能否独立于蛋白质抗原的碳骨架识别其氨基酸侧链?

Do antibodies recognize amino acid side chains of protein antigens independently of the carbon backbone?

作者信息

Van Cleave V H, Naeve C W, Metzger D W

机构信息

Department of Immunology, St. Jude Children's Research Hospital, Memphis, Tennessee 38101.

出版信息

J Exp Med. 1988 Jun 1;167(6):1841-8. doi: 10.1084/jem.167.6.1841.

Abstract

In an effort to understand the structural basis for antigen mimicry by internal image antibodies, we determined the variable (V) region sequences of two mouse mAbs that mimic the rabbit Ig a1 allotype. The results showed that while the mAb light chains did not contain any allotype-related residues, both heavy chain V regions contained within complementarity-determining region 2 an unusual sequence homologous to the nominal antigen but in opposite orientation with respect to the carbon backbone. The ability of the internal image reversed sequence to express an a1-like determinant was tested directly by producing synthetic peptides that corresponded to the presumed antigenic regions of rabbit Ig and the mAb internal images, respectively. Although the two peptides presented the homologous residues in opposite orientations, they both completely inhibited at similar concentrations the binding of rabbit Ig to anti-a1 antibody. Conservative substitutions in the peptide sequence identified a paired Thr and Glu as being critical for expression of the a1 epitope. These findings indicate that antibodies can recognize the molecular environments created by amino acid side chains independently from the orientation of the protein carbon backbone.

摘要

为了理解内影像抗体模拟抗原的结构基础,我们测定了两种模拟兔Ig a1同种异型的小鼠单克隆抗体的可变(V)区序列。结果显示,虽然单克隆抗体轻链不包含任何与同种异型相关的残基,但两条重链V区在互补决定区2中均含有一个与名义抗原同源但相对于碳骨架方向相反的异常序列。通过分别合成与兔Ig假定抗原区和单克隆抗体内影像相对应的肽段,直接测试了内影像反向序列表达a1样决定簇的能力。尽管这两个肽段以相反方向呈现同源残基,但它们在相似浓度下均完全抑制兔Ig与抗a1抗体的结合。肽序列中的保守取代确定了一对苏氨酸和谷氨酸对a1表位的表达至关重要。这些发现表明,抗体能够独立于蛋白质碳骨架的方向识别氨基酸侧链所形成的分子环境。

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