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同种特异性细胞溶解性T淋巴细胞识别杂种小鼠移植抗原上的构象决定簇。

Allospecific cytolytic T lymphocytes recognize conformational determinants on hybrid mouse transplantation antigens.

作者信息

Bluestone J A, Foo M, Allen H, Segal D, Flavell R A

出版信息

J Exp Med. 1985 Jul 1;162(1):268-81. doi: 10.1084/jem.162.1.268.

Abstract

Alloreactive cytolytic T cell (CTL) lines and clones have been used to identify the sites of polymorphism of antigens of the major histocompatibility complex (MHC). Specific CTL were generated against wild-type H-2b products by cells from H-2b mutant mice that had one or a few amino acid changes in either the alpha 1 or alpha 2 domains of the Kb or Db class I molecules. These CTL populations, which might be expected to react with determinants expressed on single MHC domains, were examined for lytic activity on L cells expressing newly constructed hybrid class I molecules. Transformed cell lines expressing native class I molecules or hybrid class I molecules in which the alpha 1 and alpha 2 domains of H-2Kb had been substituted by those domains of H-2Db were lysed by H-2Db-specific CTL. Similarly, all H-2Kb-specific CTL recognized hybrid molecules in which the alpha 1 and alpha 2 domains of H-2Kb were inserted into the H-2Db molecule. In contrast, exchange of the alpha 1 domains of H-2Kb and H-2Db resulted in a total loss of recognition by Kb and Db-specific CTL. These results suggest that the allodeterminants recognized by H-2 mutant CTL are influenced by interactions between the alpha 1 and alpha 2 domains, findings similar to those seen using conventional alloreactive T cells (11). These results were compared to the binding of alloreactive mAbs, including 5 new mAbs specific for the Kb molecules. Finally, it was shown that primary and secondary CTL responses could be generated by direct sensitization against hybrid class I molecules, demonstrating that these molecules express neoantigenic determinants recognized by alloreactive CTL.

摘要

同种异体反应性细胞毒性T细胞(CTL)系和克隆已被用于鉴定主要组织相容性复合体(MHC)抗原的多态性位点。通过来自H-2b突变小鼠的细胞产生针对野生型H-2b产物的特异性CTL,这些突变小鼠的Kb或Db I类分子的α1或α2结构域中有一个或几个氨基酸发生了变化。这些CTL群体,预期会与单个MHC结构域上表达的决定簇发生反应,被检测对表达新构建的杂交I类分子的L细胞的裂解活性。表达天然I类分子或杂交I类分子(其中H-2Kb的α1和α2结构域已被H-2Db结构域取代)的转化细胞系被H-2Db特异性CTL裂解。同样,所有H-2Kb特异性CTL都识别将H-2Kb的α1和α2结构域插入H-2Db分子中的杂交分子。相反,H-2Kb和H-2Db的α1结构域交换导致Kb和Db特异性CTL完全丧失识别能力。这些结果表明H-2突变CTL识别的同种异体决定簇受α1和α2结构域之间相互作用的影响,这一发现与使用传统同种异体反应性T细胞所观察到的结果相似(11)。将这些结果与同种异体反应性单克隆抗体(包括5种针对Kb分子的新单克隆抗体)的结合情况进行了比较。最后,结果表明通过直接致敏杂交I类分子可以产生初次和二次CTL反应,这表明这些分子表达了被同种异体反应性CTL识别的新抗原决定簇。

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