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人类免疫缺陷病毒1型(HIV-1)疫苗研发:用多包膜混合疫苗应对病毒多样性

HIV-1 vaccine development: tackling virus diversity with a multi-envelope cocktail.

作者信息

Hurwitz Julia L, Zhan Xiaoyan, Brown Scott A, Bonsignori Mattia, Stambas John, Lockey Timothy D, Sealy Robert, Surman Sherri, Freiden Pam, Jones Bart, Martin Louis, Blanchard James, Slobod Karen S

机构信息

Department of Immunology, St. Jude Children's Research Hospital, 332 N. Lauderdale, Memphis, TN 38105, USA.

出版信息

Front Biosci. 2008 Jan 1;13:609-20. doi: 10.2741/2706.

Abstract

A major obstacle to the design of a global HIV-1 vaccine is viral diversity. At present, data suggest that a vaccine comprising a single antigen will fail to generate broadly reactive B-cell and T-cell responses able to confer protection against the diverse isolates of HIV-1. While some B-cell and T-cell epitopes lie within the more conserved regions of HIV-1 proteins, many are localized to variable regions and differ from one virus to the next. Neutralizing B-cell responses may vary toward viruses with different i) antibody contact residues and/or ii) protein conformations while T-cell responses may vary toward viruses with different (i) T-cell receptor contact residues and/or (ii) amino acid sequences pertinent to antigen processing. Here we review previous and current strategies for HIV-1 vaccine development. We focus on studies at St. Jude Children's Research Hospital (SJCRH) dedicated to the development of an HIV-1 vaccine cocktail strategy. The SJCRH multi-vectored, multi-envelope vaccine has now been shown to elicit HIV-1-specific B- and T-cell functions with a diversity and durability that may be required to prevent HIV-1 infections in humans.

摘要

全球人类免疫缺陷病毒1型(HIV-1)疫苗设计的一个主要障碍是病毒的多样性。目前,数据表明,包含单一抗原的疫苗无法产生广泛反应性的B细胞和T细胞应答,从而无法对多种HIV-1分离株提供保护。虽然一些B细胞和T细胞表位位于HIV-1蛋白较为保守的区域内,但许多表位定位于可变区,并且在不同病毒之间存在差异。针对具有不同(i)抗体接触残基和/或(ii)蛋白质构象的病毒,中和性B细胞应答可能会有所不同,而针对具有不同(i)T细胞受体接触残基和/或(ii)与抗原加工相关的氨基酸序列的病毒,T细胞应答可能会有所不同。在此,我们综述了以往和当前HIV-1疫苗研发的策略。我们重点关注圣犹大儿童研究医院(SJCRH)致力于开发HIV-1疫苗组合策略的研究。SJCRH的多载体、多包膜疫苗现已显示出能够引发HIV-1特异性B细胞和T细胞功能,其多样性和持久性可能是预防人类HIV-1感染所必需的。

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