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首页> 外文期刊>The journal of immunology >Importance of Antibody in Virus Infection and Vaccine-Mediated Protection by a Latency-Deficient Recombinant Murine γ-Herpesvirus-68
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Importance of Antibody in Virus Infection and Vaccine-Mediated Protection by a Latency-Deficient Recombinant Murine γ-Herpesvirus-68

机译:抗体在病毒感染和疫苗介导的保护中的重要性在于延迟缺陷重组鼠γ-疱疹病毒-68

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The human γ-herpesviruses EBV and Kaposi’s sarcoma-associated herpesvirus establish lifelong latent infections, can reactivate in immunocompromised individuals, and are associated with the development of malignancies. Murine γ-herpesvirus-68 (γHV68), a rodent pathogen related to EBV and Kaposi’s sarcoma-associated herpesvirus, provides an important model to dissect mechanisms of immune control and investigate vaccine strategies. Infection of mice with γHV68 elicits robust antiviral immunity, and long-term protection from γHV68 reactivation requires both cellular and humoral immune responses. Vaccination of mice with AC-replication and transcription activator (RTA), a highly lytic latency-null recombinant γHV68, results in complete protection from wild-type γHV68 infection that lasts for at least 10 mo. In this report, we examine the immune correlates of AC-RTA–mediated protection and show that sterilizing immunity requires both T cells and Ab. Importantly, Ab was also critical for mitigating viral infection in the brain, and in the absence of Ab-mediated control, amplification of the AC-RTA virus in the brain resulted in fatality. Our results highlight important considerations in the development of vaccination strategies based on live-attenuated viruses.
机译:人类的γ疱疹病毒EBV和卡波西氏肉瘤相关的疱疹病毒可建立终身潜伏感染,可在免疫功能低下的个体中重新激活,并与恶性肿瘤的发生有关。鼠γ-疱疹病毒68(γHV68)是一种与EBV和卡波西氏肉瘤相关的疱疹病毒有关的啮齿动物病原体,为解剖免疫控制机制和研究疫苗策略提供了重要模型。用γHV68感染小鼠会产生强大的抗病毒免疫力,要长期保护γHV68的再激活,就需要细胞和体液免疫反应。用高度复制潜伏期无效的重组γHV68交流复制和转录激活剂(RTA)对小鼠进行疫苗接种,可完全保护其免受持续至少10 mo的野生型γHV68感染。在本报告中,我们研究了AC-RTA介导的保护作用的免疫相关性,并表明对杀菌的免疫既需要T细胞,又需要Ab。重要的是,Ab对于缓解脑部病毒感染也至关重要,在没有Ab介导的控制的情况下,脑中AC-RTA病毒的扩增会导致死亡。我们的结果突出了在基于减毒活病毒的疫苗接种策略开发中的重要考虑因素。

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