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抗原肽与H-2Kd I类主要组织相容性复合体分子的相互作用。

The interaction of antigenic peptides with the H-2Kd MHC class I molecule.

作者信息

Maryanski J L, Lüthy R, Romero P, Healy F, Drouet C, Casanova J L, Jaulin C, Kourilsky P, Corradin G

机构信息

Ludwig Institute for Cancer Research, Lausanne Branch, Epalinges, Switzerland.

出版信息

Semin Immunol. 1993 Apr;5(2):95-104. doi: 10.1006/smim.1993.1013.

Abstract

An important event in the recognition of antigen by T cells is the selective interaction of peptides with major histocompatibility complex (MHC) molecules. We have defined several critical structural features that promote the efficient interaction of antigenic peptides with the MHC class I molecule, H-2Kd. For four unrelated antigens, we found that optimal synthetic peptides were short, only 9 or 10 amino acids long. These and other H-2Kd-restricted peptides were found to share a distinct 2-residue binding motif. Two regions in the H-2Kd antigen binding site that might accommodate the motif residues were identified by analysis of Ala-substituted H-2Kd molecules. A molecular model showing the possible interaction of one antigenic peptide with the H-2Kd molecule is presented.

摘要

T细胞识别抗原过程中的一个重要事件是肽与主要组织相容性复合体(MHC)分子的选择性相互作用。我们已经确定了几个关键的结构特征,这些特征促进了抗原肽与I类MHC分子H-2Kd的有效相互作用。对于四种不相关的抗原,我们发现最佳的合成肽很短,只有9或10个氨基酸长。这些以及其他受H-2Kd限制的肽被发现共享一个独特的双残基结合基序。通过对丙氨酸取代的H-2Kd分子的分析,确定了H-2Kd抗原结合位点中可能容纳基序残基的两个区域。本文展示了一个分子模型,该模型显示了一种抗原肽与H-2Kd分子可能的相互作用。

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