Chemical genetic control of cytokine signaling in CAR-T cells using lenalidomide-controlled membrane-bound degradable IL-7.
Michael C KannEmily M SchneiderAntonio J AlmazanIsabel C LaneAmanda A BouffardValentina M SupperHana N TakeiAlexander TepperMark B LeickRebecca C LarsonBenjamin L EbertMarcela V MausMax JanPublished in: Leukemia (2023)
CAR-T cell therapy has emerged as a breakthrough therapy for the treatment of relapsed and refractory hematologic malignancies. However, insufficient CAR-T cell expansion and persistence is a leading cause of treatment failure. Exogenous or transgenic cytokines have great potential to enhance CAR-T cell potency but pose the risk of exacerbating toxicities. Here we present a chemical-genetic system for spatiotemporal control of cytokine function gated by the off-patent anti-cancer molecular glue degrader drug lenalidomide and its analogs. When co-delivered with a CAR, a membrane-bound, lenalidomide-degradable IL-7 fusion protein enforced a clinically favorable T cell phenotype, enhanced antigen-dependent proliferative capacity, and enhanced in vivo tumor control. Furthermore, cyclical pharmacologic combined control of CAR and cytokine abundance enabled the deployment of highly active, IL-7-augmented CAR-T cells in a dual model of antitumor potency and T cell hyperproliferation.
Keyphrases
- multiple myeloma
- cell therapy
- stem cell transplantation
- newly diagnosed
- acute myeloid leukemia
- induced apoptosis
- acute lymphoblastic leukemia
- stem cells
- emergency department
- diffuse large b cell lymphoma
- mesenchymal stem cells
- low dose
- microbial community
- risk assessment
- chronic lymphocytic leukemia
- cell death
- cell proliferation
- antibiotic resistance genes