Schmitt-Verhulst A M, Shearer G M
J Exp Med. 1976 Dec 1;144(6):1701-6. doi: 10.1084/jem.144.6.1701.
One of the more recent associations of the murine H-2 major histocompatibility complex (MHC) with immune function has been the finding that cytotoxic T-effector cells generated by sensitization with viral-infected (1-6), chemically modified (7-9), or weak transplantation antigen-associated (10,11) syngeneic cells can efficiently lyse target cells which express the same viral, chemical, or weak antigenic agent, and which share the H-2K and/or H-2D regions of the MHC with the responding and/or stimulating cells. Furthermore, an additional contribution of a gene(s) within the H-2 complex has been demonstrated which controls immune response potential (Ir genes) in the generation of cytotoxic effector cells to trinitrophenyl (TNP)-modified self components (12,13). In such studies it was found that certain B10 congenic strains generated good cytotoxic responses to both TNP- modified H-2K and H-2D region products, whereas other B10 congenic strains exhibited preferential or exclusive reactivity against TNP-modified H-2K region products. Some of these recombinant strains differing in response potential to TNP- modified H-2D products expressed the same haplotype at the D end, but differed at the K end of H-2. The low responsiveness observed in the B10.A strain to TNP-modified H-2D(d) when compared to B10.D2 and (B10.A x B10.D2)F(1) for the same specificity, suggested a role of dominant Ir genes which map in K, I-A, I-B, I-J, and/or I-E (12, 14). In the present report an attemnpt was made to further map within the MHC the Ir gene(s) controlling cell-mediated lympholysis (CML) to TNP-modified H-2D(d), by using recombinant mouse strains on the A and B10 backgrounds. Irrespective of the genetic background, the s and k haplotypes at the K end generated high and low cytotoxic responses, respectively, to H-2D(d)-TNP. The intermediate responder and low responder status of the A.TL and A.AL strains, respectively, indicated that a gene mapping in the K region of H-2 influences response potential. Furthermore, the differences in the levels of cytotoxicity detected in the A.TH and A.TL strains suggested an additional I region influence. Taken together these findings raise the possibility that multiple genes mapping within different regions of the MHC control the level of T-cell-mediated cytotoxicity to chemically modified autologous cells.
小鼠H-2主要组织相容性复合体(MHC)与免疫功能的最新关联之一是发现,用病毒感染的(1-6)、化学修饰的(7-9)或弱移植抗原相关的(10,11)同基因细胞致敏产生的细胞毒性T效应细胞能够有效地裂解表达相同病毒、化学物质或弱抗原剂的靶细胞,并且这些靶细胞与反应性和/或刺激性细胞共享MHC的H-2K和/或H-2D区域。此外,已证明H-2复合体内的一个基因对细胞毒性效应细胞对三硝基苯基(TNP)修饰的自身成分的产生中的免疫反应潜能(Ir基因)有额外贡献(12,13)。在这些研究中发现,某些B10同源系对TNP修饰的H-2K和H-2D区域产物均产生良好的细胞毒性反应,而其他B10同源系对TNP修饰的H-2K区域产物表现出优先或排他性反应。这些对TNP修饰的H-2D产物反应潜能不同的重组系中的一些在D端表达相同的单倍型,但在H-2的K端不同。与B10.D2和(B10.A×B10.D2)F1相比,B10.A系对TNP修饰的H-2D(d)的低反应性表明,位于K、I-A、I-B、I-J和/或I-E中的显性Ir基因起作用(12,14)。在本报告中,试图通过使用A和B10背景的重组小鼠品系,在MHC内进一步定位控制对TNP修饰的H-2D(d)的细胞介导淋巴细胞溶解(CML)的Ir基因。无论遗传背景如何,K端的s和k单倍型分别对H-2D(d)-TNP产生高和低细胞毒性反应。A.TL和A.AL品系分别为中等反应者和低反应者状态,表明位于H-2的K区域的一个基因影响反应潜能。此外,在A.TH和A.TL品系中检测到的细胞毒性水平差异表明I区域有额外影响。综合这些发现,提出了在MHC不同区域定位的多个基因控制对化学修饰自体细胞的T细胞介导细胞毒性水平的可能性。
