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      Broadly-Neutralizing Antibodies (bNAbs) for the Treatment and Prevention of HIV Infection

      research-article
      Current opinion in HIV and AIDS
      broadly neutralizing antibodies, clinical trials, HIV reservoir, HIV cure

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          Abstract

          Purpose of review:

          Several anti-HIV-1 broadly neutralizing antibodies (bNAbs) with exceptional breadth and potency and targeting different HIV-1 envelope epitopes have entered clinical trials. bNAbs are being evaluated for their potential as long-acting alternatives to antiretrovirals in HIV-1 prevention and therapy, and for potential role in strategies aiming at long-term viral remission. Here, we discuss recent findings from bNAb clinical studies.

          Recent findings:

          bNAbs targeting distinct HIV-1 envelope epitopes have shown, in general, favorable safety profiles, and engineered bNAb variants have demonstrated improved pharmacokinetics. Single bNAb infusions transiently decreased viremia with subsequent selection of escape variants, while a combination of two bNAbs successfully maintained viral suppression in individuals harboring antibody-sensitive viruses after antiretroviral therapy (ART) was discontinued. Studies in animal models suggest that bNAbs can modulate immune responses and potentially interfere with the establishment or composition of the latent reservoir, and ongoing clinical studies aim to assess potential bNAb-mediated effects on HIV-1 persistence and host immune responses.

          Summary:

          Early clinical studies support additional evaluation of bNAbs. Antibodies may offer advantages over standard ART for HIV-1 prevention and therapy, and as components of immunologic strategies to achieve sustained virologic control. The evaluation of engineered bNAbs with multi-specificity, extended half-lives and increased potency as well as alternative bNAb-delivery systems are being pursued.

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          Most cited references39

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          Broadly neutralizing anti-HIV-1 antibodies require Fc effector functions for in vivo activity.

          Broadly neutralizing antibodies (bNAbs) against HIV-1 provide both effective pre-exposure prophylaxis and treatment of HIV-1 infection in murine and nonhuman primate models, suggesting their potential use in humans. Although much is known about the role of variable domains in the neutralization breadth and potency of these bNAbs, the contribution of Fc domains to their activities is, by contrast, poorly characterized. Assessment of the in vivo activity of several bNAbs revealed that FcγR-mediated effector function contributes substantially to their capacity to block viral entry, suppress viremia, and confer therapeutic activity. Enhanced in vivo potency of anti-HIV-1 bNAbs was associated with preferential engagement of activating, but not inhibitory FcγRs, and Fc domain-engineered bNAb variants with selective binding capacity for activating FcγRs displayed augmented protective activity. These findings reveal key roles for Fc effector function in the in vivo activity of anti-HIV-1 bNAbs and provide strategies for generating bNAbs with improved efficacy. Copyright © 2014 Elsevier Inc. All rights reserved.
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            Antibodies in HIV-1 vaccine development and therapy.

            Despite 30 years of study, there is no HIV-1 vaccine and, until recently, there was little hope for a protective immunization. Renewed optimism in this area of research comes in part from the results of a recent vaccine trial and the use of single-cell antibody-cloning techniques that uncovered naturally arising, broad and potent HIV-1-neutralizing antibodies (bNAbs). These antibodies can protect against infection and suppress established HIV-1 infection in animal models. The finding that these antibodies develop in a fraction of infected individuals supports the idea that new approaches to vaccination might be developed by adapting the natural immune strategies or by structure-based immunogen design. Moreover, the success of passive immunotherapy in small-animal models suggests that bNAbs may become a valuable addition to the armamentarium of drugs that work against HIV-1.
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              Broadly neutralizing antibodies and viral inducers decrease rebound from HIV-1 latent reservoirs in humanized mice.

              Latent reservoirs of HIV-1-infected cells are refractory to antiretroviral therapies (ART) and remain the major barrier to curing HIV-1. Because latently infected cells are long-lived, immunologically invisible, and may undergo homeostatic proliferation, a "shock and kill" approach has been proposed to eradicate this reservoir by combining ART with inducers of viral transcription. However, all attempts to alter the HIV-1 reservoir in vivo have failed to date. Using humanized mice, we show that broadly neutralizing antibodies (bNAbs) can interfere with establishment of a silent reservoir by Fc-FcR-mediated mechanisms. In established infection, bNAbs or bNAbs plus single inducers are ineffective in preventing viral rebound. However, bNAbs plus a combination of inducers that act by independent mechanisms synergize to decrease the reservoir as measured by viral rebound. Thus, combinations of inducers and bNAbs constitute a therapeutic strategy that impacts the establishment and maintenance of the HIV-1 reservoir in humanized mice.
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                Author and article information

                Journal
                101264945
                34537
                Curr Opin HIV AIDS
                Curr Opin HIV AIDS
                Current opinion in HIV and AIDS
                1746-630X
                1746-6318
                9 June 2020
                January 2020
                01 January 2021
                : 15
                : 1
                : 49-55
                Affiliations
                Laboratory of Molecular Immunology, The Rockefeller University, New York, NY, USA
                Author notes
                Author of correspondence: Marina Caskey, MD. Laboratory of Molecular Immunology, The Rockefeller University, New York, NY 10065, USA. Tel:+1 212 327 7396; mcaskey@ 123456rockefeller.edu .
                Article
                PMC7340121 PMC7340121 7340121 nihpa1601642
                10.1097/COH.0000000000000600
                7340121
                31764199
                e6e68a1b-d548-4777-bb44-6504f8c0a9a3
                History
                Categories
                Article

                broadly neutralizing antibodies,clinical trials,HIV cure,HIV reservoir

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