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小鼠中对流感病毒细胞毒性T细胞反应的选择性抑制

Selective suppression of the cytotoxic T cell response to influenza virus in mice.

作者信息

Leung K, Ashman R B, Ertl H C, Ada G L

出版信息

Eur J Immunol. 1980 Nov;10(11):803-10. doi: 10.1002/eji.1830101102.

Abstract

Mice injected with inactivated (UV light-irradiated) influenza virus produce specific antibody, become sensitized for a delayed-type hypersensitivity reaction, but do not generate specific cytotoxic T (Tc) cells. If injected 4-5 days later with infectious virus, the formation of Tc cells is suppressed by > 90%. If A strain viruses are used, the suppression observed is cross-reactive within A strain viruses but does not extend to B/LEE or to Sendai virus. Serum from mice injected with UV-irradiated virus contains antibodies which on adoptive transfer can inhibit Tc cell formation when infectious homologous virus is used to challenge the recipients. Spleen cells from the same mice, upon adoptive transfer, also inhibit (50-70%) Tc cell formation if transferred within 24 h of injection of infectious virus, and the specificity pattern observed is cross-reactive within A strains. The activity of the cells mediating suppression is destroyed by monospecific anti-Thy-1.2 antibody and complement. The immune cells require I region sharing between donor and recipient mice for their suppressor activity to be effective. (There is also a partial requirement for K, D region sharing, but the possible rejection of transferred cells is not excluded.) Dilution assays in which clonal expansion of Tc precursors is used to estimate their frequency and the presence of T helper (Th) cells indicate that suppressed mice possess Tc precursors and primed cells which, upon restimulation, act as Th cells. Furthermore, injection of irradiated Th cells with inactivated virus does not significantly reduce the ensuing suppression.

摘要

注射灭活(紫外线照射)流感病毒的小鼠会产生特异性抗体,对迟发型超敏反应产生致敏作用,但不会产生特异性细胞毒性T(Tc)细胞。如果在4 - 5天后注射感染性病毒,Tc细胞的形成会被抑制90%以上。如果使用A株病毒,观察到的抑制作用在A株病毒内具有交叉反应性,但不会扩展到B/LEE株或仙台病毒。注射紫外线照射病毒的小鼠血清中含有抗体,当用感染性同源病毒攻击受体时,这些抗体通过过继转移可抑制Tc细胞的形成。来自同一小鼠的脾细胞,在注射感染性病毒后24小时内进行过继转移时,也会抑制(50 - 70%)Tc细胞的形成,并且观察到的特异性模式在A株内具有交叉反应性。介导抑制作用的细胞活性会被单特异性抗Thy - 1.2抗体和补体破坏。免疫细胞需要供体和受体小鼠之间共享I区域才能使其抑制活性有效。(对K、D区域共享也有部分要求,但不排除转移细胞可能被排斥。)使用Tc前体细胞的克隆扩增来估计其频率以及T辅助(Th)细胞存在情况的稀释试验表明,受抑制的小鼠拥有Tc前体细胞和经致敏的细胞,这些细胞在再次刺激时会作为Th细胞发挥作用。此外,用灭活病毒注射经照射的Th细胞并不会显著降低随后出现的抑制作用。

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