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基于热休克蛋白的多价疫苗靶向 HSV-2:CD4(+)和 CD8(+)细胞免疫和保护效力。

A heat shock protein based polyvalent vaccine targeting HSV-2: CD4(+) and CD8(+) cellular immunity and protective efficacy.

机构信息

Agenus Inc., Lexington, MA, USA.

出版信息

Vaccine. 2011 Nov 3;29(47):8530-41. doi: 10.1016/j.vaccine.2011.07.011. Epub 2011 Jul 19.

DOI:10.1016/j.vaccine.2011.07.011
PMID:21767588
Abstract

Efforts to develop a subunit vaccine against genital herpes have been hampered by lack of knowledge of the protective antigens of HSV-2, the causative agent of the disease. Vaccines based either on selected antigens or attenuated live virus approaches have not demonstrated meaningful clinical activity. We present here results of a therapeutic vaccine candidate, HerpV (formerly called AG-707), consisting of 32 HSV-2 peptides derived from 22 HSV-2 proteins, complexed non-covalently to the HSP70 chaperone and formulated with QS-21 saponin adjuvant. HerpV is observed to be immunogenic, generating CD4(+) and CD8(+) T cell responses in three mouse strains including HLA-A2 transgenic mice. Optimal T cell stimulation was dependent on the synergistic adjuvant properties of QS-21 with hsp70. The vaccine provided significant protection from viral challenge in a mouse prophylaxis model and showed signals of activity in a guinea pig therapeutic model of existing infection. Peripheral blood mononuclear cells from human HSV-2(+) subjects also showed reactivity in vitro to a subset of individual peptides and to the pool of all 32 peptides. Recombinant human Hsc70 complexed with the 32 peptides also stimulated the expansion of CD8(+) T cells from HSV-2(+) subjects in vitro. These studies demonstrate that HerpV is a promising immunotherapy candidate for genital herpes, and provide a foundation for evaluating HerpV in human HSV-2(+) subjects with the intent of eliciting CD4(+) and CD8(+) T cell responses to a broad array of viral antigens.

摘要

开发生殖器疱疹亚单位疫苗的努力受到缺乏对 HSV-2 保护性抗原的了解的阻碍,HSV-2 是该疾病的病原体。基于选定抗原或减毒活病毒方法的疫苗尚未显示出有意义的临床活性。我们在此介绍一种治疗性疫苗候选物 HerpV(以前称为 AG-707)的结果,该疫苗由 32 个来自 22 种 HSV-2 蛋白的 HSV-2 肽组成,与 HSP70 伴侣非共价复合物,并与 QS-21 皂苷佐剂配制。观察到 HerpV 具有免疫原性,在包括 HLA-A2 转基因小鼠在内的三种小鼠品系中产生 CD4(+)和 CD8(+) T 细胞反应。最佳 T 细胞刺激取决于 QS-21 与 hsp70 的协同佐剂特性。该疫苗在小鼠预防模型中提供了针对病毒挑战的显著保护,并在现感染的豚鼠治疗模型中显示出活性信号。来自人类 HSV-2(+)受试者的外周血单核细胞也在体外对个别肽和所有 32 个肽的混合物显示出反应性。与 32 个肽复合的重组人 Hsc70 也在体外刺激 HSV-2(+)受试者的 CD8(+)T 细胞扩增。这些研究表明 HerpV 是生殖器疱疹有前途的免疫疗法候选物,并为在人类 HSV-2(+)受试者中评估 HerpV 提供了基础,目的是引起针对广泛病毒抗原的 CD4(+)和 CD8(+)T 细胞反应。

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