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小鼠经皮钦德病毒二次感染后记忆细胞介导的免疫反应的产生。

Generation of memory cell-mediated immune responses after secondary infection of mice with pichinde virus.

作者信息

Walker C M, Rawls W E, Rosenthal K L

出版信息

J Immunol. 1984 Jan;132(1):469-74.

PMID:6317748
Abstract

Pichinde virus (PV), a member of the arenavirus group, was found to elicit strong cell-mediated immune responses in various strains of mice. After primary i.v. inoculation, augmentation of natural killer (NK) cell activity occurred and peaked 3 to 4 days after infection. The NK response was followed by a second peak of cytotoxic activity that was found to be H-2 restricted, virus specific, and mediated by Thy-1.2+, Lyt-2.2+ lymphocytes. This cytotoxic T lymphocyte (CTL) response peaked 7 days post infection. Neutralizing antibodies were not detectable after PV infection of the mice. In light of this, we investigated the generation and kinetics of secondary cell-mediated immune responses after reinjection of homologous virus in vivo. Slight but significant augmentation of NK activity was observed 1 day after secondary virus challenge. As in the primary response, effectors of this NK activity rapidly became sensitive to anti-Thy-1.2 and complement treatment. NK activity rapidly returned to background levels and was followed by an anamnestic CTL response that peaked 4 days after reinjection of the virus. Thus, cell-mediated immune responses appeared more rapidly after secondary challenge in vivo, and the temporal relationship between NK and CTL generation was maintained. Both secondary NK and CTL responses were generated in mice that had been pretreated with cyclophosphamide (CY), suggesting that memory cell-mediated immune responses can be reactivated in vivo without undergoing cell division. In contrast, treatment with CY before primary infection delayed the appearance of virus-induced NK activity and abrogated the generation of H-2-restricted virus-specific CTL. Rechallenge of these CY-treated NK-primed mice resulted in the rapid generation of a secondary NK response that was not followed by either a primary or secondary CTL response. The data suggest that cells mediating a nonspecific effector function may possess specific memory. We discuss our results with respect to possible NK-CTL relationships.

摘要

皮钦德病毒(PV)是沙粒病毒科的一员,已发现它能在多种品系的小鼠中引发强烈的细胞介导免疫反应。初次静脉注射后,自然杀伤(NK)细胞活性增强,并在感染后3至4天达到峰值。NK反应之后是细胞毒性活性的第二个峰值,该峰值被发现是H-2限制性的、病毒特异性的,且由Thy-1.2+、Lyt-2.2+淋巴细胞介导。这种细胞毒性T淋巴细胞(CTL)反应在感染后7天达到峰值。小鼠感染PV后未检测到中和抗体。鉴于此,我们研究了在体内再次注射同源病毒后二次细胞介导免疫反应的产生和动力学。二次病毒攻击后1天观察到NK活性有轻微但显著的增强。与初次反应一样,这种NK活性的效应细胞迅速变得对抗Thy-1.2和补体处理敏感。NK活性迅速恢复到背景水平,随后是再次注射病毒后4天达到峰值的回忆性CTL反应。因此,体内二次攻击后细胞介导免疫反应出现得更快,并且NK和CTL产生之间的时间关系得以维持。二次NK和CTL反应均在经环磷酰胺(CY)预处理的小鼠中产生,这表明记忆性细胞介导免疫反应可以在体内重新激活而无需经历细胞分裂。相比之下,初次感染前用CY处理会延迟病毒诱导的NK活性的出现,并消除H-2限制性病毒特异性CTL的产生。对这些经CY处理的NK启动小鼠再次攻击导致快速产生二次NK反应,随后既没有出现初次也没有出现二次CTL反应。数据表明介导非特异性效应功能的细胞可能具有特异性记忆。我们就可能的NK-CTL关系讨论了我们的结果。

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