grant

Development of Allogeneic CAR T Cell Therapy for a Functional Cure of HIV Infection

Organization MASSACHUSETTS GENERAL HOSPITALLocation BOSTON, UNITED STATESPosted 1 Mar 2022Deadline 28 Feb 2027
NIHUS FederalResearch GrantFY2026AIDS VirusAccelerationAcquired Immune Deficiency Syndrome VirusAcquired Immunodeficiency Syndrome VirusAcute B-Lymphocytic LeukemiaAllogenicAnti-Retroviral AgentsAutologousB cell progenitor acute lymphoblastic leukemiaB-ALLB-Cell Acute Lymphocytic LeukemiaB-Cell Acute Lymphoblastic LeukemiaB-Cell Lymphoblastic LeukemiaB-cell ALLB-cell precursor acute lymphoblastic leukemiaBerlinBindingBody TissuesC-C CKR-5C-C CKR-5 GeneC-C Chemokine Receptor Type 5C-C Chemokine Receptor Type 5 GeneCAR T cell therapyCAR T cellsCAR T therapyCAR modified T cellsCAR-TCAR-TsCC Chemokine Receptor 5CC-CKR-5CC-CKR-5 GeneCC-CKR5CCCKR5CCCKR5 GeneCCR-5CCR-5 GeneCCR5CCR5 ProteinCCR5 ReceptorsCCR5 geneCD19CD19 geneCD195 AntigenCD195 Antigen GeneCD28CD28 geneCD8 CellCD8 T cellsCD8 lymphocyteCD8+ T cellCD8+ T-LymphocyteCD8-Positive LymphocytesCD8-Positive T-LymphocytesCHEMR13CHEMR13 GeneCKR-5CKR-5 GeneCKR5CKR5 GeneCKR5 ReceptorsCMKBR5CMKBR5 GeneCMVCancersCardiovascular DiseasesCell BodyCellsCellular biologyCharacteristicsChemokine (C-C Motif) Receptor 5Chemokine (C-C) Receptor 5Chemokine (C-C) Receptor 5 GeneChronicClinicalClinical TrialsConsumptionCytomegalovirusDNADataDeoxyribonucleic AcidDevelopmentDiseaseDisease ProgressionDisease remissionDisorderDrugsDysfunctionExhibitsFunctional disorderGenerationsGenesGeneticHCMVHIVHIV InfectionsHIV cureHIV functional cureHIV replicationHIV treatment vaccineHIV vaccine therapyHIV viral infectionHIV viral replicationHIV virus infectionHIV-1 Fusion Co-ReceptorHIV-1 Fusion Co-Receptor GeneHIV-1 cureHIV-1 functional cureHIV-1 infectionHIV-1 replicationHIV-1 viral replicationHIV-1 virus replicationHIV/AIDS cureHeadHematopoietic Cell TumorHematopoietic MalignanciesHematopoietic NeoplasmsHematopoietic Neoplasms including LymphomasHematopoietic TumorHematopoietic and Lymphoid Cell NeoplasmHematopoietic and Lymphoid NeoplasmsHeterogeneityHumanHuman Immunodeficiency VirusesImmuneImmune responseImmune systemImmunesImmunotherapeutic agentIndividualInfectionInfection by HIV-1Infection from HIV-1Infection of HIV-1InflammationInfusionInfusion proceduresInterruptionJunk DNAKnowledgeLAV-HTLV-IIILondonLong-term infectionLymphadenopathy-Associated VirusM mulattaM. mulattaMacaca mulattaMacaca rhesusMalignant Hematopoietic NeoplasmMalignant NeoplasmsMalignant TumorMediatingMedicationModern ManModificationMolecular InteractionMorbidityPathogenesisPathogenicityPatientsPharmaceutical PreparationsPhenotypePhysiopathologyPre-B-Cell LeukemiaPrecursor B Lymphoblastic LeukemiaProductionProgenitor CellsRemissionResistanceRhesus MacaqueRhesus MonkeySIVSalivary Gland VirusesSimian Immunodeficiency VirusesSourceT cell based immune therapyT cell based therapeuticsT cell based therapyT cell directed therapiesT cell immune therapyT cell immunotherapyT cell receptor based immunotherapyT cell receptor cellular immunotherapyT cell receptor engineered therapyT cell receptor immunotherapyT cell responseT cell targeted therapeuticsT cell therapyT cell treatmentT cell-based immunotherapyT cell-based treatmentT cells for CART cellular immunotherapyT cellular therapyT lymphocyte based immunotherapyT lymphocyte based therapyT lymphocyte therapeuticT lymphocyte treatmentT-Cell DevelopmentT-Cell OntogenyT-Cell Receptor TherapyT-Cell Receptor TreatmentT-Cell Receptor based TherapyT-Cell Receptor based TreatmentT-CellsT-LymphocyteT-Lymphocyte DevelopmentT-cell therapeuticsT-cell transfer therapyT44T8 CellsT8 LymphocytesTCR T cell immunotherapyTCR T cell therapyTCR TherapyTCR based T cell immunotherapyTCR based TherapyTCR based immune therapyTCR based immunotherapyTCR based treatmentTCR immunotherapyTestingTherapeuticTimeTissuesVaccinationVariantVariationViralViral BurdenViral LoadViral Load resultViral reservoirVirusVirus reservoirVirus-HIVadoptive T cell transferadoptive T lymphocyte transferadoptive T-cell therapyallotransplantallotransplantationanti-cancer immunotherapyanti-retroviralanti-viral efficacyanticancer immunotherapyantiretroviral therapyantiretroviral treatmentbase editingblood cancercancer immunotherapycancer of bloodcancer of the bloodcardiovascular disordercell biologychallenge in rhesus macaqueschimeric antigen T cell receptorchimeric antigen receptorchimeric antigen receptor (CAR) T cell therapychimeric antigen receptor (CAR) T cellschimeric antigen receptor Tchimeric antigen receptor T cell therapychimeric antigen receptor T cellschimeric antigen receptor T therapychimeric antigen receptor fusion protein T-cellschimeric antigen receptor modified T cellschronic infectioncostcytomegalovirus groupdevelopmentaldrug/agentefficacy studyengineered T cellsfabrication costgene desertgenetically engineered T-cellshost responsehuman diseasehuman immunodeficiency virus curehuman immunodeficiency virus infectionhuman immunodeficiency virus replicationhuman immunodeficiency virus-1 replicationhumanized micehumanized mouseimmune drugsimmune system responseimmune-based cancer therapiesimmune-based therapeuticsimmunologic therapeuticsimmunoresponseimmunotherapeuticsimmunotherapy agentimmunotherapy for cancerimmunotherapy of cancerimprovedin vivoinfected rhesus macaquesinfected rhesus monkeyinfected with HIVinfected with human immunodeficiency virusinfection in rhesus macaquesinfection of rhesus macaquesinfusionsinterestmalignancymanufacturing costmortalitymouse modelmurine modelneoplasm/cancernovelpathophysiologypersistent infectionpreventpreventingprophylacticresistantresponserhesus challengerhesus macaque challengerhesus monkey infectionstem cellssuccesstherapeutic HIV vaccinationtherapeutic HIV vaccinetherapeutic T-cell platformtherapeutic vaccination against HIVthymus derived lymphocytetranscriptomicstransgenic T- cellstumorvector inducedvector-based vaccineviral reboundvirus rebound
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Full Description

Abstract: Antiretroviral therapy (ART) dramatically reduces HIV-associated morbidity and mortality (1).
However, it is not a practical cure as eradication of HIV through ART alone is estimated to require over 60 years
of treatment (1, 2). Numerous studies support that HIV-specific T cell responses are critical for efficient targeting
and elimination of HIV infected cells that are the source of chronic infection (3-10). Unfortunately, viral escape
and a limited presence of functional virus-specific effector CD8+ T cells undermine the potency of these
responses in chronically infected individuals (11-17). As such, there is growing interest in the development of
novel immunotherapeutic approaches to target and eliminate HIV-infected cells to achieve viral
suppression in the absence of ART, a “functional cure”.
Chimeric antigen receptor (CAR) T cell immunotherapies have demonstrated great promise against
blood cancers (18-20), and now also demonstrate the potential to mitigate HIV/SIV infection in rhesus macaques
(21, 22) and humanized mice (23-28). We recently showed that HIV-specific Dual CD4-based CAR T cells co-
expressing independent 4-1BB and CD28 costimulatory domains restrict HIV replication and reduce viral burden
in humanized mice (23). However, current limitations of using autologous T cells to derive CAR T cell products
(TCPs), including time-consuming and costly manufacturing, insufficient or dysfunctional patient-derived T cells,
and the inter-patient heterogeneity of TCPs, are barriers to their widespread application to human diseases.
Development of allogeneic TCPs derived from healthy human donors, could, however, provide an ‘off-the-shelf’
treatment option to overcome these hurdles, as well as accelerate the use of CAR T cell therapies (29-38).
Unfortunately, post-infusion elimination by the recipient’s immune system remains a major hurdle (39-41).
Here we propose to leverage our expertise in CAR T cell biology (21, 23, 25, 26, 42, 43), base editing
(44-49), and a humanized mouse model of HIV infection (50-58) to develop an allogeneic CAR T cell therapy
against HIV. Building on our preliminary data applying efficient multiplex base editing to CAR T cells, we
hypothesize that both base editing approaches and identification of an optimal allogenic donor will enable the
development of an allorejection-resistant CD4-based CAR TCP with enhanced efficacy to eliminate HIV-infected
cells and suppress HIV in the absence of ART. To test this hypothesis, we propose the following specific aims:
Aim 1: Determine whether genetic modifications to allogeneic T cells can augment their in vivo
persistence.
Aim 2: Identify characteristics of allogeneic HIV-specific CD4CAR T cells that associate with enhanced
persistence and antiviral efficacy.
Aim 3: Compare the in vivo HIV efficacy of allogeneic versus autologous HIV-specific CD4CAR T cells,
incorporating Aim 1 and 2’s signatures of improved allogeneic functionality.

Grant Number: 5R01AI170189-05
NIH Institute/Center: NIH
Principal Investigator: Christian Boutwell

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