Published January 2017 | Version Accepted Version
Journal Article Open

Antibody gene transfer with adeno-associated viral vectors as a method for HIV prevention

Abstract

Broadly neutralizing antibodies (bNAbs) against human immunodeficiency virus (HIV) show great promise in HIV prevention as they are capable of potently neutralizing a considerable breadth of genetically diverse strains. Passive transfer of monoclonal bNAb proteins can confer protection in animal models of HIV infection at modest concentrations, inspiring efforts to develop an HIV vaccine capable of eliciting bNAb responses. However, these antibodies demonstrate high degrees of somatic mutation and other unique characteristics that may hinder the ability of conventional approaches to consistently and effectively produce bNAb analogs. As an alternative strategy, we and others have proposed vector-mediated gene transfer to generate long-term, systemic production of bNAbs in the absence of immunization. Herein, we review the use of adeno-associated virus (AAV) vectors for delivery of HIV bNAbs and antibody-like proteins and summarize both the advantages and disadvantages of this strategy as a method for HIV prevention.

Additional Information

© 2017 John Wiley & Sons A/S. Issue online: 30 JAN 2017. Version of Record online: 30 JAN 2017. A. B. B. is supported by the National Institutes for Drug Abuse (NIDA) Avenir New Innovator Award DP2DA040254, the MGH Transformative Scholars Program as well as funding from the Charles H. Hood Foundation. This independent research was supported by the Gilead Sciences Research Scholars Program in HIV. D. B. and A. B. B. were supported by the National Institutes of Health (HHSN266200500035C) through a contract from the NIAID. There are no conflicts of interest.

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Additional details

Identifiers

PMCID
PMC5300685
Eprint ID
74069
Resolver ID
CaltechAUTHORS:20170206-091735457

Funding

NIH
DP2DA040254
Massachusetts General Hospital
Charles H. Hood Foundation
Gilead Sciences Research Scholars Program in HIV
NIH
HHSN266200500035C

Dates

Created
2017-02-06
Created from EPrint's datestamp field
Updated
2021-11-11
Created from EPrint's last_modified field