Candidate Antibody-Based Therapeutics Against HIV-1

被引:0
|
作者
Rui Gong
Weizao Chen
Dimiter S. Dimitrov
机构
[1] National Institutes of Health,Protein Interactions Group, Frederick National Laboratory for Cancer Research
来源
BioDrugs | 2012年 / 26卷
关键词
Protein Disulfide Isomerase; Palivizumab; Membrane Proximal External Region; CD4bs Antibody; CD4i Epitope;
D O I
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学科分类号
摘要
Antibody-based therapeutics have been successfully used for the treatment of various diseases and as research tools. Several well characterized, broadly neutralizing monoclonal antibodies (bnmAbs) targeting HIV-1 envelope glycoproteins or related host cell surface proteins show sterilizing protection of animals, but they are not effective when used for therapy of an established infection in humans. Recently, a number of novel bnmAbs, engineered antibody domains (eAds), and multifunctional fusion proteins have been reported which exhibit exceptionally potent and broad neutralizing activity against a wide range of HIV-1 isolates from diverse genetic subtypes. eAds could be more effective in vivo than conventional full-size antibodies generated by the human immune system. Because of their small size (12∼15 kD), they can better access sterically restricted epitopes and penetrate densely packed tissue where HIV-1 replicates than the larger full-size antibodies. HIV-1 possesses a number of mechanisms to escape neutralization by full-size antibodies but could be less likely to develop resistance to eAds. Here, we review the in vitro and in vivo antiviral efficacies of existing HIV-1 bnmAbs, summarize the development of eAds and multispecific fusion proteins as novel types of HIV-1 inhibitors, and discuss possible strategies to generate more potent antibody-based candidate therapeutics against HIV-1, including some that could be used to eradicate the virus.
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页码:143 / 162
页数:19
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