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针对HIV-1的中和抗体的中和机制及保护活性

Neutralizing antibodies mechanism of neutralization and protective activity against HIV-1.

作者信息

Xiao Yi, Dong Xiaonan, Chen Ying-Hua

机构信息

Research Centre for Medical Science, Department of Biology, Tsinghua University, Beijing, P.R. China.

出版信息

Immunol Res. 2002;25(3):193-200. doi: 10.1385/IR:25:3:193.

Abstract

The role of the humoral immune response in prevention against HIV-1 infection is still incompletely understood. However, neutralizing antibodies to certain epitopes on HIV-1 envelope glycoproteins inhibit HIV-1 infection in vitro and in vivo. Passive administration of these antibodies by themselves or in combination completely protected hu-PBL-SCID mice or macaques from intravenous, vaginal, as well as maternal-fetal mucosal transmission. All these studies provide direct experimental evidence that neutralizing antibodies are potent enough to prevent HIV infection, and strongly suggest that neutralizing-antibody-based vaccines could provide effective protection against HIV-1, despite the potent action of CTLs. Some neutralizing epitopes have been defined in vitro and in vivo. Unfortunately, none of the neutralizing-antibody-based candidate vaccines has been demonstrated to induce enough protective activity. Weak antigenicity and immunogenicity of neutralizing epitopes on native or recombinant proteins and other factors made it difficult to induce neutralizing-epitope-specific antibody responses in vivo enough to prevent against primary isolates. Recent studies indicated that HIV-1 variations resulted in escape from neutralization or the CTL responses, which may be the principal challenge for HIV-1 prevention. Epitope vaccine as a new strategy activating both arms of the immune system, namely, using the "principal neutralizing epitopes" and the CTL epitopes in combination, should provide new hope for developing an effective vaccine to halt the HIV-1 epidemic.

摘要

体液免疫反应在预防HIV-1感染中的作用仍未完全明确。然而,针对HIV-1包膜糖蛋白某些表位的中和抗体在体外和体内均可抑制HIV-1感染。单独或联合被动给予这些抗体可使hu-PBL-SCID小鼠或猕猴完全免受静脉内、阴道内以及母婴黏膜传播的感染。所有这些研究都提供了直接的实验证据,表明中和抗体足以预防HIV感染,并强烈提示基于中和抗体的疫苗尽管受到CTL的强力作用,但仍可提供针对HIV-1的有效保护。一些中和表位已在体外和体内得到明确。不幸的是,尚无基于中和抗体的候选疫苗被证明能诱导足够的保护活性。天然或重组蛋白上中和表位的弱抗原性和免疫原性以及其他因素使得在体内难以诱导足以预防原始分离株的中和表位特异性抗体反应。最近的研究表明,HIV-1变异导致中和或CTL反应逃逸,这可能是HIV-1预防的主要挑战。表位疫苗作为一种激活免疫系统两个分支的新策略,即联合使用“主要中和表位”和CTL表位,应为开发有效的疫苗以阻止HIV-1流行带来新的希望。

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