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How Can HIV-Type-1-Env Immunogenicity Be Improved to Facilitate Antibody-Based Vaccine Development?

机译:如何改善HIV 1-Env免疫原性以促进基于抗体的疫苗开发?

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摘要

No vaccine candidate has induced antibodies (Abs) that efficiently neutralize multiple primary isolates of HIV-1. Preexisting high titers of neutralizing antibodies (NAbs) are essential, because the virus establishes infection before anamnestic responses could take effect. HIV-1 infection elicits Abs against Env, Gag, and other viral proteins, but of these only a subset of the anti-Env Abs can neutralize the virus. Whereas the corresponding proteins from other viruses form the basis of successful vaccines, multiple large doses of HIV-1 Env elicit low, transient titers of Abs that are not protective in humans. The inaccessibility of neutralization epitopes hinders NAb induction, but Env may also subvert the immune response by interacting with receptors on T cells, B cells, monocytes, macrophages, and dendritic cells. Here, we discuss evidence from immunizations of different species with various modified Env constructs. We also suggest how the divergent Ab responses to Gag and Env during infection may reflect differences in B cell regulation. Drawing on these analyses, we outline strategies for improving Env as a component of a vaccine aimed at inducing strong and sustained NAb responses.
机译:没有候选疫苗可以诱导抗体(Abs)有效中和HIV-1的多个主要分离株。预先存在高滴度的中和抗体(NAbs)是必不可少的,因为该病毒会在记忆消除反应生效之前就开始感染。 HIV-1感染会引发针对Env,Gag和其他病毒蛋白的Abs,但其中只有一部分抗Env Abs可以中和病毒。尽管来自其他病毒的相应蛋白质构成成功疫苗的基础,但多次大剂量的HIV-1 Env会引起对人体无保护作用的低,短暂的抗体滴度。中和表位的不可及性阻碍了NAb的诱导,但是Env也可能通过与T细胞,B细胞,单核细胞,巨噬细胞和树突状细胞上的受体相互作用来破坏免疫应答。在这里,我们讨论了用各种修饰的Env构建体免疫不同物种的证据。我们还建议感染期间对Gag和Env的不同Ab反应如何反映B细胞调节的差异。借助这些分析,我们概述了改善Env的策略,该策略旨在诱导强而持续的NAb应答的疫苗。

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