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被低估的慢病毒模型:HIV-2 研究能为开发有效的 HIV-1 疫苗做出什么贡献?

An underestimated lentivirus model: what can HIV-2 research contribute to the development of an effective HIV-1 vaccine?

机构信息

Nuffield Department of Medicine, University of Oxford, Oxford, OX3 9DS, UK.

出版信息

Expert Rev Anti Infect Ther. 2011 Feb;9(2):195-206. doi: 10.1586/eri.10.176.

DOI:10.1586/eri.10.176
PMID:21342067
Abstract

The development of an HIV-1 vaccine that would be effective against all existing subtypes and circulating recombinant forms remains one of the great scientific and public health challenges of our generation. One of the major barriers to HIV-1 vaccine development is a lack of understanding of the correlates of protective immunity against the virus. In this context, research has focused on the rare phenomenon of spontaneous control of HIV-1 infection, in groups referred to as 'long-term nonprogressors' and 'elite controllers', together with models of nonprogressive sooty mangabey simian immunodeficiency (SIV) infection in African nonhuman primate hosts such as sooty mangabeys and African green monkeys, in which the majority of animals tolerate high levels of viral replication without development of immunodeficiency or disease. Much less attention has been given to humans infected with the nonpandemic strain HIV-2, derived from the SIV in West Africa, most of whom behave as long-term nonprogressors or viral controllers, while a minority develop disease clinically indistinguishable from AIDS caused by HIV-1. This apparent dichotomous outcome is, based on the evidence accumulated to date, more clearly related to the host immune response than the good clinical outcome of HIV-1 controllers. We propose that complementing research into HIV-1 controllers and nonpathogenic SIV models with the prioritization of HIV-2 research could enhance the HIV-1 vaccine research effort. The absence of disease progression or detectable plasma viral replication in the presence of an effective immune response in most patients living with HIV-2 represents an opportunity to unravel the virus' evolutionary adaptation in human hosts and to establish the correlates of such a protective response.

摘要

开发一种能够针对所有现有亚型和循环重组形式的 HIV-1 疫苗仍然是我们这一代人面临的重大科学和公共卫生挑战之一。阻碍 HIV-1 疫苗开发的主要障碍之一是缺乏对保护性免疫病毒的相关因素的了解。在这种情况下,研究集中在 HIV-1 感染的自发控制的罕见现象上,在被称为“长期非进展者”和“精英控制器”的群体中,以及在非人类灵长类动物中非进展性黑猩猩猴免疫缺陷病毒(SIV)感染的模型中,大多数动物可以容忍高水平的病毒复制,而不会出现免疫缺陷或疾病。人们对感染非大流行株 HIV-2 的人类关注较少,该病毒源自西非的 SIV,其中大多数人表现为长期非进展者或病毒控制器,而少数人则表现出与 HIV-1 引起的艾滋病临床无法区分的疾病。基于迄今为止积累的证据,这种明显的二分法结果与宿主免疫反应的关系比 HIV-1 控制器的良好临床结果更为密切。我们建议,将 HIV-1 控制器和非致病性 SIV 模型的研究与 HIV-2 研究的优先化相结合,可以增强 HIV-1 疫苗研究的力度。在大多数感染 HIV-2 的患者中,存在有效的免疫反应,但没有疾病进展或可检测到的血浆病毒复制,这代表了一个机会,可以揭示病毒在人类宿主中的进化适应,并确定这种保护反应的相关因素。

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