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迈向无症状临床疱疹疫苗的合理设计:旧知、新知与未知

Towards a rational design of an asymptomatic clinical herpes vaccine: the old, the new, and the unknown.

作者信息

Chentoufi Aziz Alami, Kritzer Elizabeth, Yu David M, Nesburn Anthony B, Benmohamed Lbachir

机构信息

Laboratory of Cellular and Molecular Immunology, School of Medicine, University of California, Irvine, Irvine, CA 92697-4375, USA.

出版信息

Clin Dev Immunol. 2012;2012:187585. doi: 10.1155/2012/187585. Epub 2012 Mar 26.

Abstract

The best hope of controlling the herpes simplex virus type 1 and type 2 (HSV-1 and HSV-2) pandemic is the development of an effective vaccine. However, in spite of several clinical trials, starting as early as 1920s, no vaccine has been proven sufficiently safe and efficient to warrant commercial development. In recent years, great strides in cellular and molecular immunology have stimulated creative efforts in controlling herpes infection and disease. However, before moving towards new vaccine strategy, it is necessary to answer two fundamental questions: (i) why past herpes vaccines have failed? (ii) Why the majority of HSV seropositive individuals (i.e., asymptomatic individuals) are naturally "protected" exhibiting few or no recurrent clinical disease, while other HSV seropositive individuals (i.e., symptomatic individuals) have frequent ocular, orofacial, and/or genital herpes clinical episodes? We recently discovered several discrete sets of HSV-1 symptomatic and asymptomatic epitopes recognized by CD4(+) and CD8(+) T cells from seropositive symptomatic versus asymptomatic individuals. These asymptomatic epitopes will provide a solid foundation for the development of novel herpes epitope-based vaccine strategy. Here we provide a brief overview of past clinical vaccine trials, outline current progress towards developing a new generation "asymptomatic" clinical herpes vaccines, and discuss future mucosal "asymptomatic" prime-boost vaccines that could optimize local protective immunity.

摘要

控制1型和2型单纯疱疹病毒(HSV - 1和HSV - 2)大流行的最大希望是开发一种有效的疫苗。然而,尽管早在20世纪20年代就开始了多项临床试验,但尚未有疫苗被证明足够安全和有效,足以保证进行商业化开发。近年来,细胞和分子免疫学取得了巨大进展,激发了在控制疱疹感染和疾病方面的创新努力。然而,在转向新的疫苗策略之前,有必要回答两个基本问题:(i)过去的疱疹疫苗为何失败?(ii)为什么大多数HSV血清阳性个体(即无症状个体)能自然“受到保护”,很少或没有复发性临床疾病,而其他HSV血清阳性个体(即有症状个体)却频繁出现眼部、口腔和/或生殖器疱疹临床发作?我们最近发现了几组离散的HSV - 1有症状和无症状表位,它们可被血清阳性有症状个体与无症状个体的CD4(+)和CD8(+) T细胞识别。这些无症状表位将为开发基于疱疹表位的新型疫苗策略提供坚实基础。在此,我们简要概述过去的临床疫苗试验,概述开发新一代“无症状”临床疱疹疫苗的当前进展,并讨论未来可优化局部保护性免疫的黏膜“无症状”初免 - 加强疫苗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/33ac/3324142/9527d223f87f/CDI2012-187585.001.jpg

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