Assessing the impact of AGS-004, a dendritic cell-based immunotherapy, and vorinostat on persistent HIV-1 Infection

Joann Kuruc ,David M Margolis,Alicia Gamble,Robert J Gorelick,Joseph J Eron,Brigitte Allard,Erin Stuelke,Morgan Dewey ,Mark Debenedette ,Joanna Warren ,Michael G Hudgens ,Jennifer Kirchherr ,Katherine S James ,Charles A Nicolette,Ana Plachco,Sarah A Reifeis,Carolina Garrido,Alyson Helms,Irina Y Tcherepanova,Shane D Falcinelli,Nancie M Archin,Nilu Goonetilleke

doi:10.1038/s41598-020-61878-3

Abstract

Approaches to deplete persistent HIV infection are needed. We investigated the combined impact of the latency reversing agent vorinostat (VOR) and AGS-004, an autologous dendritic cell immunotherapeutic, on the HIV reservoir. HIV+, stably treated participants in whom resting CD4+ T cell-associated HIV RNA (rca-RNA) increased after VOR exposure ex vivo and in vivo received 4 doses of AGS-004 every 3 weeks, followed by VOR every 72 hours for 30 days, and then the cycle repeated. Change in VOR-responsive host gene expression, HIV-specific T cell responses, low-level HIV viremia, rca-RNA, and the frequency of resting CD4+ T-cell infection (RCI) was measured at baseline and after each cycle. No serious treatment-related adverse events were observed among five participants. As predicted, VOR-responsive host genes responded uniformly to VOR dosing. Following cycles of AGS-004 and VOR, rca-RNA decreased significantly in only two participants, with a significant decrease in SCA observed in one of these participants. However, unlike other cohorts dosed with AGS-004, no uniform increase in HIV-specific immune responses following vaccination was observed. Finally, no reproducible decline of RCI, defined as a decrease of >50%, was observed. AGS-004 and VOR were safe and well-tolerated, but no substantial impact on RCI was measured. In contrast to previous clinical data, AGS-004 did not induce HIV-specific immune responses greater than those measured at baseline. More efficacious antiviral immune interventions, perhaps paired with more effective latency reversal, must be developed to clear persistent HIV infection.

Highlights

Life-long antiretroviral therapy (ART) is required to prevent rebound of viremia and return of disease, due to the persistence of long-lived viral reservoirs
Given the theoretical risks of vorinostat, and the low likelihood of clinical benefit in this study, we first confirmed ex vivo exposure to VOR resulted in a measurable increase in resting CD4+ T cell-associated HIV ribonucleic acid (RNA) (rca-RNA) in the resting CD4+ T cells of participants from a donation provided after screening
If a significant increase in rca-RNA was observed after the paired dose, the participants went on to receive the combination of VOR and AGS-004

Summary

Introduction

Life-long antiretroviral therapy (ART) is required to prevent rebound of viremia and return of disease, due to the persistence of long-lived viral reservoirs. AGS-004 is a dendritic cell (DC)-based immunotherapy consisting of matured autologous DCs co-electroporated with in vitro transcribed ribonucleic acid (RNA) encoding autologous HIV antigens (gag, vpr, rev, and nef) plus synthetically derived cluster of differentiation 40 ligand (CD40L) RNA to achieve DC functionality[10]. This vaccine was reported to induce HIV-specific effector/memory CD8 T-cell responses in HIV-infected individuals who had initiated ART during acute or chronic infection[11,12,13]. In this study we investigated the impact of VOR combined with AGS-004, on persistent HIV infection

Methods

Results

Conclusion