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用于评估疫苗接种中第一靶细胞的缺陷型巨细胞病毒。

A spread-deficient cytomegalovirus for assessment of first-target cells in vaccination.

机构信息

Max von Pettenkofer Institute, Ludwig Maximilians University, Pettenkoferstrasse 9a, Munich, Germany.

出版信息

J Virol. 2010 Aug;84(15):7730-42. doi: 10.1128/JVI.02696-09. Epub 2010 May 12.

DOI:10.1128/JVI.02696-09
PMID:20463067
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2897632/
Abstract

Human cytomegalovirus (HCMV) is a human pathogen that causes severe disease primarily in the immunocompromised or immunologically immature individual. To date, no vaccine is available. We describe use of a spread-deficient murine CMV (MCMV) as a novel approach for betaherpesvirus vaccination. To generate a spread-deficient MCMV, the conserved, essential gene M94 was deleted. Immunization with MCMV-DeltaM94 is apathogenic and protective against wild-type challenge even in highly susceptible IFNalphabetaR(-/-) mice. MCMV-DeltaM94 was able to induce a robust CD4(+) and CD8(+) T-cell response as well as a neutralizing antibody response comparable to that induced by wild-type infection. Endothelial cells were identified as activators of CD8(+) T cells in vivo. Thus, the vaccination with a spread-deficient betaherpesvirus is a safe and protective strategy and allows the linkage between cell tropism and immunogenicity. Furthermore, genomes of MCMV-DeltaM94 were present in lungs 12 months after infection, revealing first-target cells as sites of genome maintenance.

摘要

人类巨细胞病毒(HCMV)是一种人类病原体,主要在免疫功能低下或免疫不成熟的个体中引起严重疾病。迄今为止,尚无疫苗可用。我们描述了使用传播缺陷型鼠巨细胞病毒(MCMV)作为β疱疹病毒疫苗接种的新方法。为了产生传播缺陷型 MCMV,缺失了保守的、必需的基因 M94。用 MCMV-DeltaM94 免疫是无毒的,并且即使在高度易感的 IFNalphabetaR(-/-)小鼠中也能预防野生型攻击。MCMV-DeltaM94 能够诱导强大的 CD4(+)和 CD8(+)T 细胞反应以及中和抗体反应,与野生型感染诱导的反应相当。内皮细胞被鉴定为体内 CD8(+)T 细胞的激活剂。因此,用传播缺陷型β疱疹病毒进行疫苗接种是一种安全且有保护作用的策略,并允许将细胞嗜性与免疫原性联系起来。此外,MCMV-DeltaM94 的基因组在感染 12 个月后仍存在于肺部,揭示了最初的靶细胞作为基因组维持的部位。

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