首页> 外文OA文献 >Immune response gene function correlates with the expression of an Ia antigen. I. Preferential association of certain Ae and E alpha chains results in a quantitative deficiency in expression of an Ae:E alpha complex
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Immune response gene function correlates with the expression of an Ia antigen. I. Preferential association of certain Ae and E alpha chains results in a quantitative deficiency in expression of an Ae:E alpha complex

机译:免疫应答基因功能与1a抗原的表达相关。 I.某些Ae和E alpha链的优先结合会导致Ae:E alpha复合物表达的定量不足

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摘要

These studies were stimulated by the observation, reported in the accompanying paper (19), that IEu failed to interact with I-Ak or I-As in F1 mice to allow a response to the antigen, pigeon cytochrome c, unlike I-E subregions derived from other Ia.7+ haplotypes. Serological and biochemical analyses were performed to determine whether or not cells from these F1 mice express the Ak,se:E alpha complexes that should function as restriction elements for T cell recognition of pigeon cytochrome c on antigen-presenting cells. Using the Y-17 monoclonal antibody, which recognizes the combinatorial or conformational determinant Ia.m44 on certain Ae:E alpha complexes, we were able to distinguish between Aue:Eu alpha and Ab,k,se:Eu alpha complexes on cell surfaces. Although complement-dependent microcytotoxicity with Y-17 failed to detect Ab,k,se:Eu alpha complexes on cells from appropriate F1 mice, these molecules were detected by both quantitative absorption and quantitative immunofluorescence studies. However, Ab,k,se:Eu alpha complexes were found to be present at levels only one-seventh to one-eighth the levels expressed by homozygous I-Ab, I-Ek; I-Ak, I-Ek; and I-As, I-Ek cells. The results of two-dimensional polyacrylamide gel electrophoresis analyses suggest that the low levels of expression of Ab,k,se:Eu alpha complexes are a consequence of the preferential association of Aue and Eu alpha chains with each other in the F1 cells. As will be shown in the following paper (19), the quantitative deficiency in the expression of Ake:Eu alpha and Ase:Eu alpha complexes results in a corresponding defect in antigen-presenting cell function, thus providing strong evidence that Ia antigens represent products of Ir genes.
机译:随同论文报道的观察结果激发了这些研究(19),即IEu无法与F1小鼠中的I-Ak或I-As相互作用以允许对抗原(鸽子细胞色素c)做出反应,这与源自其他Ia.7 +单倍型。进行了血清学和生化分析,以确定来自这些F1小鼠的细胞是否表达Ak,se:Eα复合物,该复合物应作为抗原呈递细胞上鸽细胞色素c的T细胞识别的限制元件。使用Y-17单克隆抗体,该抗体识别某些Ae:E alpha复合物上的组合或构象决定簇Ia.m44,我们能够区分细胞表面上的Aue:Eu alpha和Ab,k,se:Eu alpha复合物。尽管使用Y-17的补体依赖性微细胞毒性未能检测到适当F1小鼠细胞上的Ab,k,se:Eu alpha复合物,但通过定量吸收和定量免疫荧光研究均检测到了这些分子。然而,发现Ab,k,se:Eu alpha复合物的水平仅为纯合I-Ab,I-Ek表达水平的七分之一至八分之一;我知道,我知道;和I-As,I-Ek细胞。二维聚丙烯酰胺凝胶电泳分析的结果表明,Ab,k,se:Euα复合物的低水平表达是Aue和Euα链在F1细胞中相互优先结合的结果。如以下论文(19)所示,Ake:Eu alpha和Ase:Eu alpha复合物表达的定量不足会导致抗原呈递细胞功能发生相应的缺陷,从而有力证据表明Ia抗原代表了产物Ir基因。

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