Adeno-associated virus gene delivery of broadly neutralizing antibodies as prevention and therapy against HIV-1

被引:0
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作者
Allen Lin
Alejandro B. Balazs
机构
[1] Ragon Institute of MGH,Department of Systems Biology
[2] MIT and Harvard,undefined
[3] Harvard University,undefined
来源
Retrovirology | / 15卷
关键词
Vectored delivery; Antibody gene transfer; AAV; HIV-1; bNAb; Clinical trials; Animal models;
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摘要
Vectored gene delivery of HIV-1 broadly neutralizing antibodies (bNAbs) using recombinant adeno-associated virus (rAAV) is a promising alternative to conventional vaccines for preventing new HIV-1 infections and for therapeutically suppressing established HIV-1 infections. Passive infusion of single bNAbs has already shown promise in initial clinical trials to temporarily decrease HIV-1 load in viremic patients, and to delay viral rebound from latent reservoirs in suppressed patients during analytical treatment interruptions of antiretroviral therapy. Long-term, continuous, systemic expression of such bNAbs could be achieved with a single injection of rAAV encoding antibody genes into muscle tissue, which would bypass the challenges of eliciting such bNAbs through traditional vaccination in naïve patients, and of life-long repeated passive transfers of such biologics for therapy. rAAV delivery of single bNAbs has already demonstrated protection from repeated HIV-1 vaginal challenge in humanized mouse models, and phase I clinical trials of this approach are underway. Selection of which individual, or combination of, bNAbs to deliver to counter pre-existing resistance and the rise of escape mutations in the virus remains a challenge, and such choices may differ depending on use of this technology for prevention versus therapy.
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