Systematically optimized BCMA/CS1 bispecific CAR-T cells robustly control heterogeneous multiple myeloma

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作者
Eugenia Zah
Eunwoo Nam
Vinya Bhuvan
Uyen Tran
Brenda Y. Ji
Stanley B. Gosliner
Xiuli Wang
Christine E. Brown
Yvonne Y. Chen
机构
[1] University of California–Los Angeles,Department of Chemical and Biomolecular Engineering
[2] University of California–Los Angeles,Department of Chemistry and Biochemistry
[3] City of Hope Beckman Research Institute and Medical Center,Department of Hematology and Hematopoietic Cell Transplantation, T Cell Therapeutics Research Laboratory
[4] University of California–Los Angeles,Department of Microbiology, Immunology, and Molecular Genetics
[5] Parker Institute for Cancer Immunotherapy Center at UCLA,undefined
[6] Amgen,undefined
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Chimeric antigen receptor (CAR)-T cell therapy has shown remarkable clinical efficacy against B-cell malignancies, yet marked vulnerability to antigen escape and tumor relapse exists. Here we report the rational design and optimization of bispecific CAR-T cells with robust activity against heterogeneous multiple myeloma (MM) that is resistant to conventional CAR-T cell therapy targeting B-cell maturation antigen (BCMA). We demonstrate that BCMA/CS1 bispecific CAR-T cells exhibit superior CAR expression and function compared to T cells that co-express individual BCMA and CS1 CARs. Combination therapy with anti–PD-1 antibody further accelerates the rate of initial tumor clearance in vivo, while CAR-T cell treatment alone achieves durable tumor-free survival even upon tumor re-challenge. Taken together, the BCMA/CS1 bispecific CAR presents a promising treatment approach to prevent antigen escape in CAR-T cell therapy against MM, and the vertically integrated optimization process can be used to develop robust cell-based therapy against novel disease targets.
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