Bispecific BCMA/CD24 CAR-T cells control multiple myeloma growth.
Fumou SunYan ChengVisanu WanchaiWancheng GuoDavid MeryHongwei XuDongzheng GaiEric Robb SiegelClyde BaileyTimothy Cody AshbySamer Al HadidiCarolina D SchinkeSharmilan ThanendrarajanYupo MaQing YiRobert Z OrlowskiMaurizio ZangariFrits Van RheeSiegfried JanzGail A BishopGuido TricotJohn D ShaughnessyFenghuang ZhanPublished in: Nature communications (2024)
Anti-multiple myeloma B cell maturation antigen (BCMA)-specific chimeric antigen receptor (CAR) T-cell therapies represent a promising treatment strategy with high response rates in myeloma. However, durable cures following anti-BCMA CAR-T cell treatment of myeloma are rare. One potential reason is that a small subset of minimal residual myeloma cells seeds relapse. Residual myeloma cells following BCMA-CAR-T-mediated treatment show less-differentiated features and express stem-like genes, including CD24. CD24-positive myeloma cells represent a large fraction of residual myeloma cells after BCMA-CAR-T therapy. In this work, we develop CD24-CAR-T cells and test their ability to eliminate myeloma cells. We find that CD24-CAR-T cells block the CD24-Siglec-10 pathway, thereby enhancing macrophage phagocytic clearance of myeloma cells. Additionally, CD24-CAR-T cells polarize macrophages to a M1-like phenotype. A dual-targeted BCMA-CD24-CAR-T exhibits improved efficacy compared to monospecific BCMA-CAR-T-cell therapy. This work presents an immunotherapeutic approach that targets myeloma cells and promotes tumor cell clearance by macrophages.