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MHC I类分子α螺旋残基具有强同种抗原性。

Strong alloantigenicity of the alpha-helices residues of the MHC class I molecule.

作者信息

Noun G, Reboul M, Abastado J P, Kourilsky P, Sigaux F, Pla M

机构信息

Mouse Immunogenetics, U462, Institut National de la Santé et de la Recherche Médicale, Institute of Hematology, Paris, France.

出版信息

J Immunol. 1998 Jul 1;161(1):148-53.

PMID:9647218
Abstract

To evaluate the role of single residues of a MHC class I molecule in the induction of a primary allogeneic response, we have tested the ability of various point mutants (of the alpha-helices or beta-sheet of the alpha1 and alpha2 domains) of the Kd molecule to induce a primary cytotoxic T cell response in mice carrying the wild-type molecule. For that, we have used an in vivo model in which cells expressing mutant molecules were injected into the hind footpads of mice carrying wild-type Kd, and the recipient graft-draining popliteal lymph nodes were tested for the presence of alloreactive CTL. Under these experimental conditions, only 7 of the 25 mutant Kd molecules induced a primary allogeneic response. All of these mutations (positions 62, 65, 69, 72, 155, 163, 166) concern residues of the alpha-helices, demonstrating that very small variances from self in a class I molecule, located outside the peptide-binding groove, can be antigenic. To determine the peptide requirements for the generation of a primary allogeneic response, we have analyzed the repertoire of peptides selected by individual mutant molecules shown to be able or unable to induce a CTL response. No correlation was observed between the peptidic make-up presented by a given mutant and its capacity to induce a primary allogeneic response. On the whole, our data point to the alloantigenicity of potentially TCR-contacting surface residues of the MHC class I molecules.

摘要

为了评估MHC I类分子单个残基在诱导初次同种异体反应中的作用,我们测试了Kd分子的各种点突变体(α1和α2结构域的α螺旋或β折叠)在携带野生型分子的小鼠中诱导初次细胞毒性T细胞反应的能力。为此,我们使用了一种体内模型,将表达突变分子的细胞注射到携带野生型Kd的小鼠后足垫中,并检测受体移植物引流的腘窝淋巴结中是否存在同种异体反应性CTL。在这些实验条件下,25个突变Kd分子中只有7个诱导了初次同种异体反应。所有这些突变(第62、65、69、72、155、163、166位)都涉及α螺旋的残基,表明I类分子中位于肽结合槽之外的与自身的微小差异也可能具有抗原性。为了确定产生初次同种异体反应所需的肽,我们分析了已证明能够或不能诱导CTL反应的单个突变分子所选择的肽库。未观察到给定突变体呈现的肽组成与其诱导初次同种异体反应的能力之间存在相关性。总体而言,我们的数据表明MHC I类分子潜在的与TCR接触的表面残基具有同种异体抗原性。

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