抗 HIV-1 的中和抗体:我们能否用疫苗诱导产生,需要多少?
Neutralizing antibodies against HIV-1: can we elicit them with vaccines and how much do we need?
出版信息
Curr Opin HIV AIDS. 2009 Sep;4(5):347-51. doi: 10.1097/COH.0b013e32832f4a4d.
Abstract
PURPOSE OF REVIEW
This review describes some of the major obstacles that have impeded progress in the development of an effective neutralizing antibody-based HIV-1 vaccine and explains why it may be possible to overcome these obstacles. A renewed interest in the B-cell response in HIV-1-infected individuals is emphasized.
RECENT FINDINGS
New assay technologies and access to large numbers of clinical specimens have permitted a detailed assessment of the neutralizing antibody response in HIV-1-infected individuals. Recent studies have demonstrated that B cells can be stimulated to generate high titers of broadly cross-reactive neutralizing antibodies against multiple genetic subtypes of the virus. Preliminary evidence suggests that some of these antibodies are directed against epitopes in the CD4 binding site on monomeric gp120, whereas many others are directed against epitopes that remain to be identified.
SUMMARY
The rationale for pursuing an effective neutralizing antibody-based HIV-1 vaccine is strengthened by the recent demonstration of potent neutralizing antibody responses in a subset of HIV-1-infected individuals. Information on how this response develops and what epitopes are targeted could provide the insights that are needed to design improved vaccine strategies.
摘要
目的综述
本文描述了一些阻碍 HIV-1 有效中和抗体疫苗开发的主要障碍,并解释了为什么这些障碍可能会被克服。强调了重新关注 HIV-1 感染者的 B 细胞反应。
最近的发现
新的检测技术和大量临床标本的获得,使得对 HIV-1 感染者中和抗体反应进行详细评估成为可能。最近的研究表明,B 细胞可以被刺激产生针对病毒多种遗传亚型的高滴度广谱交叉中和抗体。初步证据表明,其中一些抗体针对单体 gp120 上的 CD4 结合位点表位,而许多其他抗体针对的表位仍有待确定。
总结
最近在一部分 HIV-1 感染者中展示出有效的中和抗体反应,为研发有效的基于中和抗体的 HIV-1 疫苗提供了更强的理论依据。关于该反应如何发展以及针对哪些表位的信息,可能为设计改进的疫苗策略提供所需的见解。
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