人巨细胞病毒IE1外显子4和IE2外显子5的融合蛋白在痘苗病毒疫苗载体中刺激产生强大的细胞免疫。
A fusion protein of HCMV IE1 exon4 and IE2 exon5 stimulates potent cellular immunity in an MVA vaccine vector.
作者信息
Wang Z, Zhou W, Srivastava T, La Rosa C, Mandarino A, Forman S J, Zaia J A, Britt W J, Diamond D J
机构信息
Laboratory of Vaccine Research, Division of Virology, Beckman Research Institute of the City of Hope, California 91010, USA.
出版信息
Virology. 2008 Aug 1;377(2):379-90. doi: 10.1016/j.virol.2008.04.034. Epub 2008 Jun 5.
Abstract
A therapeutic CMV vaccine incorporating an antigenic repertoire capable of eliciting a cellular immune response has yet to be successfully implemented for patients who already have acquired an infection. To address this problem, we have developed a vaccine candidate derived from modified vaccinia Ankara (MVA) that expresses three immunodominant antigens (pp65, IE1, IE2) from CMV. The novelty of this vaccine is the fusion of two adjacent exons from the immediate-early region of CMV, their successful expression in MVA, and robust immunogenicity in both primary and memory response models. Evaluation of the immunogenicity of the viral vaccine in mouse models shows that it can stimulate primary immunity against all three antigens in both the CD4(+) and CD8(+) T cell subsets. Evaluation of human PBMC from healthy CMV-positive donors or patients within 6 months of receiving hematopoietic cell transplant shows robust stimulation of existing CMV-specific CD4(+) and CD8(+) T cell subsets.
摘要
一种包含能够引发细胞免疫反应的抗原库的治疗性巨细胞病毒(CMV)疫苗,尚未成功应用于已感染CMV的患者。为了解决这一问题,我们开发了一种源自安卡拉痘苗病毒(MVA)的候选疫苗,该疫苗表达CMV的三种免疫显性抗原(pp65、IE1、IE2)。这种疫苗的新颖之处在于CMV即刻早期区域两个相邻外显子的融合、它们在MVA中的成功表达以及在初次和记忆反应模型中的强大免疫原性。在小鼠模型中对该病毒疫苗免疫原性的评估表明,它可以刺激CD4(+)和CD8(+) T细胞亚群针对所有三种抗原产生初次免疫。对健康CMV阳性供体或接受造血细胞移植后6个月内的患者的人外周血单个核细胞(PBMC)的评估显示,现有CMV特异性CD4(+)和CD8(+) T细胞亚群受到强烈刺激。
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