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重组痘苗病毒表达的鼠巨细胞病毒非结构立即早期蛋白pp89的细胞溶解性T淋巴细胞识别

Cytolytic T lymphocyte recognition of the murine cytomegalovirus nonstructural immediate-early protein pp89 expressed by recombinant vaccinia virus.

作者信息

Volkmer H, Bertholet C, Jonjić S, Wittek R, Koszinowski U H

出版信息

J Exp Med. 1987 Sep 1;166(3):668-77. doi: 10.1084/jem.166.3.668.

DOI:10.1084/jem.166.3.668
PMID:3040884
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2188685/
Abstract

The murine immediate-early (IE) protein pp89 is a nonstructural virus-encoded phosphoprotein residing in the nucleus of infected cells, where it acts as transcriptional activator. Frequency analysis has shown that in BALB/c mice the majority of virus-specific CTL recognize IE antigens. The present study was performed to assess whether pp89 causes membrane antigen expression detected by IE-specific CTL. Site-directed mutagenesis has been used to delete the introns from gene ieI, encoding pp89, for subsequent integration of the continuous coding sequence into the vaccinia virus genome. After infection with the vaccinia recombinant, the authentic pp89 was expressed in cells that became susceptible to lysis by an IE-specific CTL clone. Priming of mice with the vaccinia recombinant sensitized polyclonal CTL that recognized MCMV-infected cells and transfected cells expressing pp89. Thus, a herpesviral IE polypeptide with essential function in viral transcriptional regulation can also serve as a dominant antigen for the specific CTL response of the host.

摘要

小鼠即刻早期(IE)蛋白pp89是一种由病毒编码的非结构磷蛋白,存在于受感染细胞的细胞核中,在那里它作为转录激活因子发挥作用。频率分析表明,在BALB/c小鼠中,大多数病毒特异性CTL识别IE抗原。本研究旨在评估pp89是否会导致IE特异性CTL检测到的膜抗原表达。已使用定点诱变从编码pp89的ieI基因中删除内含子,以便随后将连续编码序列整合到痘苗病毒基因组中。用痘苗重组体感染后,在易被IE特异性CTL克隆裂解的细胞中表达了真实的pp89。用痘苗重组体对小鼠进行致敏,可使多克隆CTL识别感染MCMV的细胞和表达pp89的转染细胞。因此,一种在病毒转录调控中具有重要功能的疱疹病毒IE多肽也可作为宿主特异性CTL反应的主要抗原。

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