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H-2Ld与人类β2微球蛋白的结合会在α1和α2超结构域中诱导局部构象变化。

The association of H-2Ld with human beta-2 microglobulin induces localized conformational changes in the alpha-1 and -2 superdomain.

作者信息

Nieto M C, Song E S, McKinney D, McMillan M, Goodenow R S

机构信息

Department of Cell and Molecular Biology, University of California, Berkeley 94720.

出版信息

Immunogenetics. 1989;30(5):361-9. doi: 10.1007/BF02425276.

DOI:10.1007/BF02425276
PMID:2478461
Abstract

We have analyzed changes in the antigenicity of major histocompatibility complex class I molecules resulting from the association of human beta-2 micro-globulin (B2m) with the mouse class I heavy chain. In particular, the H-2Ld molecule exhibited enhanced cross-reactivity for the 34-1-2 monoclonal antibody. In order to assess the nature of this structural alteration induced by human B2m, we utilized H-2 class I hybrid molecules in the mapping of the 34-1-2 determinant to the helical region of the alpha-1 domain. H-2Ld class I hybrid molecules were then used to establish the importance of the alpha-2 and -3 domains in the observed increase of 34-1-2 cross-reactivity following exchange with human B2m. The H-2Ld hybrids suggest that alterations in interdomain contact are responsible for enhanced 34-1-2 cross-reactivity on the H-2Ld molecule. It is likely that this alteration arises through changes in class I conformation at regions of the molecule distant from points of contact between B2m and the class I molecule. This suggests that perturbations induced by association of human B2m with H-2Ld can affect the conformation of the alpha-1 and -2 superdomain. That class I antigenic determinants are altered by the association of human B2m with mouse class I further suggests that the class I molecule is structurally flexible and may reflect the ability of the class I molecule to bind and present a vast array of disparate peptides to the T-cell receptor.

摘要

我们分析了人类β2微球蛋白(B2m)与小鼠I类重链结合后导致的主要组织相容性复合体I类分子抗原性的变化。特别是,H-2Ld分子对34-1-2单克隆抗体表现出增强的交叉反应性。为了评估人类B2m诱导的这种结构改变的性质,我们利用H-2 I类杂交分子将34-1-2决定簇定位到α1结构域的螺旋区域。然后使用H-2Ld I类杂交分子来确定α2和α3结构域在与人类B2m交换后观察到的34-1-2交叉反应性增加中的重要性。H-2Ld杂交分子表明,结构域间接触的改变是H-2Ld分子上34-1-2交叉反应性增强的原因。这种改变可能是由于I类分子构象在远离B2m与I类分子接触点的区域发生变化而引起的。这表明人类B2m与H-2Ld结合诱导的扰动会影响α1和α2超结构域的构象。人类B2m与小鼠I类结合导致I类抗原决定簇发生改变,这进一步表明I类分子在结构上具有灵活性,可能反映了I类分子结合并向T细胞受体呈递大量不同肽段的能力。

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本文引用的文献

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