Abstract

TheabsenceofacureforHIV-1afterantiretroviraltherapyimpartsmultipleburdenstotheinfectedindividual (stigma, criminalization, life-long therapy), US society (continued infections, internal health care costs, PEPFAR), industry (pricing versus access, capacity for world-wide drug production), and global resource governance (UNAIDS, AIDS orphans, Global Fund, effects of declining economy on country/region HIV therapyprograms,etc.)justifyingafocusedinvestmentinidentifyingnovelstrategiestoachieveacureand/or stable remission after HIV infection. The BEAT-HIV Delaney Collaboratory to cure HIV-1 infection by combination immunotherapy has three central objectives. First, identify the best approach to target immunotherapy against replication competent reservoirs by defining the relationship between plasma and tissueclonalexpansion,characterizeintegrationsiteswithinbloodandtissue,anddeterminehowtomaximize viral reactivation of distinct reservoir compartments. Second, test clinical strategy combining IFN-? immunotherapy to activate intrinsic/innate responses and ADCC with broadly neutralizing anti-HIV antibodies (both strategies shown to have an effect in humans when used singly);? advance preclinical studies on IFN- alpha response, ex vivo combinations with added T-cell-mediated strategies, and develop innovative DNA vaccine delivery systems for sustaining neutralizing antibodies in vivo. Third, test clinical strategy that combines two gene therapy vectors to intrinsically protect HIV-specific killer cells by a ?CCR5 zinc nuclease given together with a CAR delivering HIV-specificity to CD8 T-cells;? advance the preclinical humanized mice platformtotestnovelcombinationsofimmunotherapy(with/withoutnoveldelivery)whenadministeredjointlyor insequencewiththeobjectivetorecruitmaximalintrinsic,innate,and/oradaptiveanti-HIVeffects.Objectives are supported by four support teams addressing Clinical, HIV reservoir measures, HIV evasion analysis, and BiostatisticsandDataManagement.Communityengagementtakesadvantageofa20+yearrelationshipwith the local HIV community, CFAR, and ACTG activity ensuring partnership with target populations. Central administration of resources will ensure maintenance of high impact milestones, study team communications, and yearly goal-oriented resource allocation and/or redistribution as informed by an executive committee, externaladvisoryboard,andNIHprogram.Asagroup,webringdiverseexpertiseandinnovationrepresenting the first time that distinct immunotherapy strategies with initial promising results in human trials focused on intrinsic/innate,humoralandadaptivearmsoftheimmuneresponseareactivelyjoinedtoadvanceanHIVcure and/orremissionunderasinglecommonmulti-investigator,multi-industryteam.Theentireteamiscommitted toadvancethebestoutcomesfromourcollectiveefforttoultimatelydevelopastrategytoeradicateHIV.

Public Health Relevance

Theinabilityofantiretroviraltherapy(ART)toclearHIVinfection,andtheobservationthatasterilizingcure and/orstableremissioncanbeachievedbyasubsetART-treatedpersonshasgalvanizedtheinterestto advanceclinicalstrategiestowardsacureand/orstableremission.Herewewillbuildonclinicalpreliminary datafromseveralsingleagentimmunotherapyhumantrialsthatindicateapotentialtoinhibitHIVbeyondART. Includingscientistsfrom8Institutionsand4Industrypartners,theBEAT-HIVDelaneyCollaboratorywillseek todevelopandtestinnovativecombinedimmunotherapystrategiestoeradicateand/orpermanentlysuppress HIVintoremissionintheabsenceofART.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project with Complex Structure Cooperative Agreement (UM1)
Project #
5UM1AI126620-03
Application #
9511758
Study Section
Special Emphasis Panel (ZAI1)
Program Officer
Mcdonald, David Joseph
Project Start
2016-07-14
Project End
2021-06-30
Budget Start
2018-07-01
Budget End
2019-06-30
Support Year
3
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Wistar Institute
Department
Type
DUNS #
075524595
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Sengupta, Srona; Siliciano, Robert F (2018) Targeting the Latent Reservoir for HIV-1. Immunity 48:872-895
Maldini, Colby R; Ellis, Gavin I; Riley, James L (2018) CAR T cells for infection, autoimmunity and allotransplantation. Nat Rev Immunol 18:605-616
Papasavvas, Emmanouil; Lada, Steven M; Joseph, Jocelin et al. (2018) Analytical ART interruption does not irreversibly change pre-interruption levels of cellular HIV. AIDS :
Szaniawski, Matthew A; Spivak, Adam M; Cox, James E et al. (2018) SAMHD1 Phosphorylation Coordinates the Anti-HIV-1 Response by Diverse Interferons and Tyrosine Kinase Inhibition. MBio 9:
Cohn, Lillian B; da Silva, Israel T; Valieris, Renan et al. (2018) Clonal CD4+ T cells in the HIV-1 latent reservoir display a distinct gene profile upon reactivation. Nat Med 24:604-609
Spivak, Adam M; Planelles, Vicente (2018) Novel Latency Reversal Agents for HIV-1 Cure. Annu Rev Med 69:421-436
Veenhuis, Rebecca T; Kwaa, Abena K; Garliss, Caroline C et al. (2018) Long-term remission despite clonal expansion of replication-competent HIV-1 isolates. JCI Insight 3:
Mendoza, Pilar; Gruell, Henning; Nogueira, Lilian et al. (2018) Combination therapy with anti-HIV-1 antibodies maintains viral suppression. Nature 561:479-484
Lada, Steven M; Huang, Karissa; VanBelzen, D Jake et al. (2018) Quantitation of Integrated HIV Provirus by Pulsed-Field Gel Electrophoresis and Droplet Digital PCR. J Clin Microbiol 56:
Lu, Ching-Lan; Pai, Joy A; Nogueira, Lilian et al. (2018) Relationship between intact HIV-1 proviruses in circulating CD4+ T cells and rebound viruses emerging during treatment interruption. Proc Natl Acad Sci U S A 115:E11341-E11348

Showing the most recent 10 out of 44 publications