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Development of an epitope-based HIV-1 vaccine strategy from HIV-1 lipopeptide to dendritic-based vaccines

机译:从HIV-1脂肽到树突式疫苗的基于表位的HIV-1疫苗策略的发展

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Introduction: Development of a safe, effective and globally affordable Human Immunodeficiency Virus strain 1 (HIV-1) vaccine offers the best hope for future control of the HIV-1 pandemic. However, with the exception of the recent RV144 trial, which elicited a modest level of protection against infection, no vaccine candidate has shown efficacy in preventing HIV-1 infection or in controlling virus replication in humans. There is also a great need for a successful immunotherapeutic vaccine since combination antiretroviral therapy (cART) does not eliminate the reservoir of HIV-infected cells. But to date, no vaccine candidate has proven to significantly alter the natural history of an individual with HIV-1 infection.Areas covered: For over 25years, the ANRS (France Recherche Nord&Sud Sida-HIV hepatites) has been committed to an original program combining basic science and clinical research developing an epitope-based vaccine strategy to induce a multiepitopic cellular response against HIV-1. This review describes the evolution of concepts, based on strategies using HIV-1 lipopeptides towards the use of dendritic cell (DC) manipulation.Expert commentary: Understanding the crucial role of DCs in immune responses allowed moving from the non-specific administration of HIV-1 sequences with lipopeptides to DC-based vaccines. These DC-targeting strategies should improve HIV-1 vaccine efficacy.
机译:简介:开发安全,有效和全球经济实惠的人免疫缺陷病毒菌株1(HIV-1)疫苗为未来控制HIV-1大流行提供了最佳希望。然而,除了最近的RV144试验中,这引发了对感染的适度保护水平,疫苗候选疫苗在预防HIV-1感染或控制人类中的病毒复制方面没有显示出疗效。由于组合抗逆转录病毒治疗(推车),也存在成功免疫治疗疫苗的需求并不能消除艾滋病毒感染细胞的储层。但到目前为止,疫苗候选人已被证明是为了显着改变艾滋病毒1感染的个体的自然历史。覆盖:超过25年,ANRS(法国Recherche Nord&Sud Sida-HIV肝寄生)一直致力于一个原始计划组合基础科学与临床研究开发基于表位的疫苗策略,诱导对HIV-1的多态性细胞反应。本综述描述了概念的演变,基于使用HIV-1脂肽的策略在使用树突状细胞(DC)操纵中.Expert评论:了解DCS在免疫应答中的关键作用允许从非特异性艾滋病毒施用用脂肽的1个序列与基于DC的疫苗。这些直流靶向策略应提高HIV-1疫苗疗效。

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