Zinkernagel R M
J Exp Med. 1976 Oct 1;144(4):933-45. doi: 10.1084/jem.144.4.933.
During infection with lymphocytic choriomeningitis or vaccinia virus, F1 irradiation chimeras reconstituted with bone marrow cells from or both parents generate cytotoxic T cells which can lyse targets across the H-2 barrier. However, activity of chimera T cells is H-2 restricted as shown by cold target competition experiments and selective restimulation of a secondary response in vitro; T cells of H-2k specificity which lyse tolerated infected H-2d target cells do not lyse infected H-2k or unrelated target cells and vice versa. Therefore, H-2 restriction of virus-specific cytotoxic T cells probably does not reflect need for like-like self-interactions for lysis to occur. The specificity of virus immune T cells is thus determined by the H-2K and H-2D specificities present in the infected animal and which are probably recognized unidirectionally by T cells. The results are compatible with the idea the T cells are specific for "altered alloantigen", i.e., a complex of cell surface marker and viral antigen. Alternatively, explained with a dual recognition model, T cells may possess two independently, clonally expressed receptors, a self-recognizer which is expressed for one of the syngeneic or tolerated allogeneic K or D "self" markers, and an immunologically specific receptor for viral antigen.
在感染淋巴细胞性脉络丛脑膜炎病毒或痘苗病毒期间,用来自一方或双方亲代的骨髓细胞重建的F1辐射嵌合体产生细胞毒性T细胞,这些细胞毒性T细胞能够裂解跨越H-2屏障的靶细胞。然而,嵌合体T细胞的活性受到H-2限制,这在冷靶竞争实验和体外二次应答的选择性再刺激中得到了证明;具有H-2k特异性的T细胞能够裂解耐受感染的H-2d靶细胞,但不能裂解感染的H-2k靶细胞或无关靶细胞,反之亦然。因此,病毒特异性细胞毒性T细胞的H-2限制可能并不反映细胞裂解发生时对相似自身相互作用的需求。病毒免疫T细胞的特异性因此由感染动物中存在的H-2K和H-2D特异性决定,并且这些特异性可能被T细胞单向识别。这些结果与T细胞对“改变的同种异体抗原”具有特异性的观点一致,即细胞表面标志物和病毒抗原的复合物。或者,用双重识别模型来解释,T细胞可能拥有两个独立的、克隆表达的受体,一个自我识别受体,它针对同基因或耐受的同种异体K或D“自我”标志物之一表达,以及一个针对病毒抗原的免疫特异性受体。