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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Evidence for a domain-swapped CD4 dimer as the coreceptor for binding to class II MHC.
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Evidence for a domain-swapped CD4 dimer as the coreceptor for binding to class II MHC.

机译:域交换CD4二聚体作为与II类MHC结合的共受体的证据。

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摘要

CD4 is a coreceptor for binding of T cells to APC and the primary receptor for HIV. The disulfide bond in the second extracellular domain (D2) of CD4 is reduced on the cell surface, which leads to formation of disulfide-linked homodimers. A large conformational change must take place in D2 to allow for formation of the disulfide-linked dimer. Domain swapping of D2 is the most likely candidate for the conformational change leading to formation of two disulfide-bonds between Cys130 in one monomer and Cys159 in the other one. Mild reduction of the extracellular part of CD4 resulted in formation of disulfide-linked dimers, which supports the domain-swapped model. The functional significance of dimer formation for coreceptor function was tested using cells expressing wild-type or disulfide-bond mutant CD4. Eliminating the D2 disulfide bond markedly impaired CD4's coreceptor function. Modeling of the complex of the TCR and domain-swapped CD4 dimer bound to class II MHC and Ag supports the domain-swapped dimer as the immune coreceptor. The known involvement of D4 residues Lys318 and Gln344 in dimer formation is also accommodated by this model. These findings imply that disulfide-linked dimeric CD4 is the preferred coreceptor for binding to APC.
机译:CD4是T细胞与APC和HIV的主要受体结合的共受体。 CD4的第二个胞外域(D2)中的二硫键在细胞表面被还原,这导致二硫键连接的同型二聚体的形成。 D2中必须发生较大的构象变化,以形成二硫键连接的二聚体。 D2的结构域交换是构象变化的最可能候选者,其构象变化导致一个单体中的Cys130与另一单体中的Cys159之间形成两个二硫键。 CD4胞外部分的轻度减少导致形成二硫键连接的二聚体,这支持结构域交换模型。使用表达野生型或二硫键突变型CD4的细胞测试了二聚体形成对共受体功能的功能意义。消除D2二硫键会明显削弱CD4的共受体功能。与II类MHC和Ag结合的TCR和结构域交换的CD4二聚体复合物的模型支持结构域交换的二聚体作为免疫共受体。该模型还容纳了D4残基Lys318和Gln344参与二聚体形成的已知过程。这些发现暗示二硫键连接的二聚体CD4是与APC结合的优选的共受体。

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