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A new set of monoclonal antibodies to human MHC class II alpha chains demonstrates that most alpha epitopes are inaccessible on the living cell surface.

机译:一组新的针对人类MHC II类α链的单克隆抗体证明大多数α表位在活细胞表面上不可接近。

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摘要

When mice were immunized with a mixture of human MHC class II alpha and beta glycoprotein chains, the predominant antibody response was anti-alpha, and from a subsequent fusion experiment over 60 hybridomas showing anti-alpha activity were generated, compared with 11 anti-beta secretors. These findings contrast with the relative paucity of anti-alpha monoclonals described previously. Use of a miniaturized Western blot screening protocol was a critical factor in the present study since the anti-alpha monoclonals do not bind to the surface of living B cells and would therefore be missed in conventional screening assays. After glutaraldehyde fixation of target B lymphocytes or B-cell lines, the majority of anti-alpha monoclonals do react in a radio-immunobinding assay, although none binds as strongly as pan-reactive anti-beta chain antibodies. This suggests that the immunogenic epitopes of alpha chains are normally concealed by the three-dimensional folding of the alpha beta dimer. The anti-alpha monoclonals were all monomorphic but varied in the extent of their reactivity with alpha chains separated on one-dimensional and two-dimensional IEF gels. The most reactive antibodies identified up to seven distinct components among mature class II antigens from solubilized cell membranes.
机译:当用人类MHC II类α和β糖蛋白链的混合物免疫小鼠时,主要的抗体反应是抗α抗体,随后的融合实验产生了60多个显示抗α活性的杂交瘤,而11种抗β抗体分泌者。这些发现与先前描述的相对较少的抗α单克隆抗体形成对比。在本研究中,使用微型Western blot筛选方案是一个关键因素,因为抗α单克隆抗体不与活B细胞表面结合,因此在常规筛选分析中会被遗漏。戊二醛固定目标B淋巴细胞或B细胞系后,大多数抗α单克隆抗体会在放射免疫结合测定中发生反应,尽管没有一个抗体能像泛反应性抗β链抗体那样牢固地结合。这表明α链的免疫原性表位通常被αβ二聚体的三维折叠所掩盖。抗α单克隆抗体都是单态的,但它们与在一维和二维IEF凝胶上分离的α链的反应程度有所不同。最活跃的抗体从溶解的细胞膜中鉴定出成熟的II类抗原中多达七个不同的成分。

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