T细胞αβ受体的轮廓结构。
The outline structure of the T-cell alpha beta receptor.
作者信息
Chothia C, Boswell D R, Lesk A M
机构信息
MRC Laboratory of Molecular Biology, Cambridge, UK.
出版信息
EMBO J. 1988 Dec 1;7(12):3745-55. doi: 10.1002/j.1460-2075.1988.tb03258.x.
Abstract
From an analysis of the immunoglobulins of known structure we derive a list of 40 sites crucial for the conserved structure of the variable domains. We show that, with marginal exceptions, the sequences of the T-cell alpha beta receptors contain, at sites homologous to these 40, the same or very similar residues. Thus the V alpha-V beta dimer has a framework structure very close to that of the immunoglobulins. Further comparisons show that parts of the surface of the V alpha-V beta framework are hypervariable. They also show that the loops that form the antigen-binding site are similar in size to those commonly found in the immunoglobulins but have different conformations. Only limited sequence variations occur in the first loop of the antigen-binding site in both V alpha and V beta. This, and their geometrical arrangement, suggest that they mainly interact with the MHC proteins.
摘要
通过对已知结构的免疫球蛋白进行分析,我们得出了40个对可变结构域保守结构至关重要的位点列表。我们发现,除了极少数例外情况,T细胞αβ受体的序列在与这40个位点同源的位置含有相同或非常相似的残基。因此,Vα-Vβ二聚体具有与免疫球蛋白非常接近的框架结构。进一步比较表明,Vα-Vβ框架表面的部分区域是高变的。这些比较还表明,形成抗原结合位点的环在大小上与免疫球蛋白中常见的环相似,但构象不同。在Vα和Vβ的抗原结合位点的第一个环中仅出现有限的序列变异。这一点及其几何排列表明,它们主要与MHC蛋白相互作用。
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