Literature DB >> 31697648

In vivo delivery of synthetic DNA-encoded antibodies induces broad HIV-1-neutralizing activity.

Megan C Wise1, Ziyang Xu2,3, Edgar Tello-Ruiz2, Charles Beck4, Aspen Trautz2, Ami Patel2, Sarah Tc Elliott2, Neethu Chokkalingam2, Sophie Kim2, Melissa G Kerkau4, Kar Muthumani2, Jingjing Jiang1, Paul D Fisher1, Stephany J Ramos1, Trevor Rf Smith1, Janess Mendoza1, Kate E Broderick1, David C Montefiori5, Guido Ferrari4, Daniel W Kulp2, Laurent M Humeau1, David B Weiner2.   

Abstract

Interventions to prevent HIV-1 infection and alternative tools in HIV cure therapy remain pressing goals. Recently, numerous broadly neutralizing HIV-1 monoclonal antibodies (bNAbs) have been developed that possess the characteristics necessary for potential prophylactic or therapeutic approaches. However, formulation complexities, especially for multiantibody deliveries, long infusion times, and production issues could limit the use of these bNAbs when deployed, globally affecting their potential application. Here, we describe an approach utilizing synthetic DNA-encoded monoclonal antibodies (dmAbs) for direct in vivo production of prespecified neutralizing activity. We designed 16 different bNAbs as dmAb cassettes and studied their activity in small and large animals. Sera from animals administered dmAbs neutralized multiple HIV-1 isolates with activity similar to that of their parental recombinant mAbs. Delivery of multiple dmAbs to a single animal led to increased neutralization breadth. Two dmAbs, PGDM1400 and PGT121, were advanced into nonhuman primates for study. High peak-circulating levels (between 6 and 34 μg/ml) of these dmAbs were measured, and the sera of all animals displayed broad neutralizing activity. The dmAb approach provides an important local delivery platform for the in vivo generation of HIV-1 bNAbs and for other infectious disease antibodies.

Entities:  

Keywords:  AIDS/HIV; Gene therapy; Immunology; Immunotherapy

Year:  2020        PMID: 31697648      PMCID: PMC6994112          DOI: 10.1172/JCI132779

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  47 in total

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