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灭活全艾滋病毒疫苗;采用一种成熟的抗病毒疫苗策略。

Killed whole-HIV vaccine; employing a well established strategy for antiviral vaccines.

作者信息

Kang C Yong, Gao Yong

机构信息

Department of Microbiology and Immunology, Schulich School of Medicine and Dentistry, The University of Western Ontario, London, ON, N6G 2V4, Canada.

出版信息

AIDS Res Ther. 2017 Sep 12;14(1):47. doi: 10.1186/s12981-017-0176-5.

Abstract

The development of an efficient prophylactic HIV vaccine has been one of the major challenges in infectious disease research during the last three decades. Here, we present a mini review on strategies employed for the development of HIV vaccines with an emphasis on a well-established vaccine technology, the killed whole-virus vaccine approach. Recently, we reported an evaluation of the safety and the immunogenicity of a genetically modified and killed whole-HIV-1 vaccine designated as SAV001 [1]. HIV-1 Clade B NL4-3 was genetically modified by deleting the nef and vpu genes and substituting the coding sequence of the Env signal peptide with that of honeybee melittin to produce an avirulent and replication efficient HIV-1. This genetically modified virus (gmHIV-1 ) was propagated in a human T cell line followed by virus purification and inactivation by aldrithiol-2 and γ-irradiation. We found that SAV001 was well tolerated with no serious adverse events. HIV-1 -specific polymerase chain reaction showed no evidence of vaccine virus replication in participants receiving SAV001 and in human T cells infected in vitro. Furthermore, SAV001 with an adjuvant significantly increased the antibody response to HIV-1 structural proteins. Moreover, antibodies in the plasma from these vaccinations neutralized tier I and tier II of HIV-1 B, A, and D subtypes. These results indicated that the killed whole-HIV vaccine is safe and may trigger appropriate immune responses to prevent HIV infection. Utilization of this killed whole-HIV vaccine strategy may pave the way to develop an effective HIV vaccine.

摘要

在过去三十年中,开发一种高效的预防性HIV疫苗一直是传染病研究中的主要挑战之一。在此,我们对HIV疫苗开发所采用的策略进行简要综述,重点关注一种成熟的疫苗技术——灭活全病毒疫苗方法。最近,我们报道了对一种名为SAV001的基因改造灭活全HIV-1疫苗的安全性和免疫原性的评估[1]。通过删除nef和vpu基因,并将Env信号肽的编码序列替换为蜜蜂蜂毒肽的编码序列,对HIV-1 B亚型NL4-3进行基因改造,以产生一种无毒且复制高效的HIV-1。这种基因改造病毒(gmHIV-1 )在人T细胞系中繁殖,随后进行病毒纯化,并用2-氨荒酸乙汞和γ射线照射进行灭活。我们发现SAV001耐受性良好,没有严重不良事件。HIV-1 特异性聚合酶链反应显示,在接受SAV001的参与者和体外感染的人T细胞中没有疫苗病毒复制的证据。此外,添加佐剂的SAV001显著增强了对HIV-1结构蛋白的抗体反应。而且,这些疫苗接种者血浆中的抗体中和了HIV-1 B、A和D亚型的I级和II级毒株。这些结果表明,灭活全HIV疫苗是安全的,可能引发适当的免疫反应以预防HIV感染。利用这种灭活全HIV疫苗策略可能为开发有效的HIV疫苗铺平道路。

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