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H-2Db或H-2Kd产物在杀伤性T淋巴细胞与同基因H-2b或H-2d病毒性淋巴瘤之间相互作用中的特异性参与。

Exclusive involvement of H-2Db or H-2Kd product in the interaction between T-killer lymphocytes and syngeneic H-2b or H-2d viral lymphomas.

作者信息

Gomard E, Duprez V, Reme T, Colombani M J, Levy J P

出版信息

J Exp Med. 1977 Oct 1;146(4):909-22. doi: 10.1084/jem.146.4.909.

Abstract

It was demonstrated previously that the cytolysis of murine viral lymphoma cells by anti-murine sarcoma virus (MSV) syngeneic T-killer lymphocytes was restricted by some products of the H-2 complex. The respective role of the products of different regions of the H-2 complex were studied with six H-2(b) and three H-2(d) lymphomas induced by five different type C viruses. They were tested in a classical chromium release test against anti-MSV T-killer cells obtained from different inbred strains of mice, including several H-2 recombinants. Tumors o pound the H-2(b) haplotype were lysed only when effectors and target cells have in common the D(b) region. On the contrary an identity limited to the K end of the H-2 complex is necessary and sufficient in the H-2(d) haplotype. An in vitro restimulation of the spleen cells with concanavalin A strongly increased the activity of in vivo-primed T lymphocytes but did not provide any response for in vivo-primed but nonresponder cells. Preincubation of the tumor cells with anti-H-2 sera abolished the lysis by syngeneic anti-MSV effector lymphocytes. The same results were obtained by preincubating the H-2(b) targets with anti-H-2D(b), or the H-2(d) target with anti-H-2K(d). Preincubation with anti-H-2K(b) or anti- H-2D(d) were ineffective. These results show that the T-killer/target cells interaction in the MSV system involved some products of the H-2 complex which might be different with the various H-2 haplotypes and could possibly vary according to the antigenic specificity. A specific association of a viral product with a normal cellular structure, directed by the H-2 region during the viral budding could explain the observed results.

摘要

先前已证明,抗鼠肉瘤病毒(MSV)同基因T杀伤淋巴细胞对鼠病毒性淋巴瘤细胞的细胞溶解作用受H-2复合体某些产物的限制。利用由五种不同的C型病毒诱导产生的六种H-2(b)和三种H-2(d)淋巴瘤,研究了H-2复合体不同区域产物的各自作用。在经典的铬释放试验中,用从不同近交系小鼠(包括几种H-2重组体)获得的抗MSV T杀伤细胞对它们进行了检测。只有当效应细胞和靶细胞具有相同的D(b)区域时,H-2(b)单倍型的肿瘤才会被溶解。相反,在H-2(d)单倍型中,H-2复合体K端的同一性是必要且充分的。用刀豆球蛋白A对脾细胞进行体外再刺激,可强烈增强体内致敏T淋巴细胞的活性,但对体内致敏但无反应的细胞则无任何反应。用抗H-2血清对肿瘤细胞进行预孵育,可消除同基因抗MSV效应淋巴细胞的溶解作用。用抗H-2D(b)对H-2(b)靶细胞进行预孵育,或用抗H-2K(d)对H-2(d)靶细胞进行预孵育,也可得到相同的结果。用抗H-2K(b)或抗H-2D(d)进行预孵育则无效。这些结果表明,MSV系统中T杀伤细胞/靶细胞的相互作用涉及H-2复合体的某些产物,这些产物可能因不同的H-2单倍型而异,并且可能根据抗原特异性而有所不同。病毒出芽过程中由H-2区域指导的病毒产物与正常细胞结构的特异性结合可以解释所观察到的结果。

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