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γ-secretase inhibitors augment efficacy of BCMA-targeting bispecific antibodies against multiple myeloma cells without impairing T-cell activation and differentiation

by Yu, Tengteng , Xing, Lijie , Aardalen, Kimberly , Munshi, Nikhil , Oka, Adwait , Cho, Shih-Feng , Lam, Joni , Chen, Hailin , Wen, Kenneth , Lin, Liang , Daley, Mike , Lu, Haihui , Anderson, Kenneth C , Tai, Yu-Tzu

in Antibodies / Antigens / Biomedical research / Cancer therapies / Cloning / Cytotoxicity / Drug dosages / Hematology / Hospitals / Immunotherapy / Laboratory animals / Lymphocytes / Medicine / Multiple myeloma / Patients / Variance analysis

2022

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γ-secretase inhibitors augment efficacy of BCMA-targeting bispecific antibodies against multiple myeloma cells without impairing T-cell activation and differentiation

2022

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γ-secretase inhibitors augment efficacy of BCMA-targeting bispecific antibodies against multiple myeloma cells without impairing T-cell activation and differentiation

2022

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Journal Article

γ-secretase inhibitors augment efficacy of BCMA-targeting bispecific antibodies against multiple myeloma cells without impairing T-cell activation and differentiation

Yu, Tengteng,

Xing, Lijie,

Aardalen, Kimberly,

Munshi, Nikhil,

Oka, Adwait,

Cho, Shih-Feng,

Lam, Joni,

Chen, Hailin,

Wen, Kenneth,

Lin, Liang,

Daley, Mike,

Lu, Haihui,

Anderson, Kenneth C,

Tai, Yu-Tzu

2022

Overview

We here defined the impacts of γ-secretase inhibitors (GSIs) on T-cell-dependent BCMA-specific multiple myeloma (MM) cell lysis and immunomodulatory effects induced by bispecific antibodies (BisAbs). GSIs-induced membrane BCMA (mBCMA) accumulation reached near maximum within 4 h and sustained over 42h-study period on MM cell lines and patient MM cells. GSIs, i.e., 2 nM LY-411575 or 1 μM DAPT, robustly increased mBCMA densities on CD138+ but not CD3+ patient cells, concomitantly with minimum soluble/shed BCMA (sBCMA) in 1 day-culture supernatants. In ex vivo MM-T-cell co-cultures, GSIs overcame sBCMA-inhibited MM cell lysis and further enhanced autologous patient MM cell lysis induced by BCMAxCD3 BisAbs, accompanied by significantly enhanced cytolytic markers (CD107a, IFNγ, IL2, and TNFα) in patient T cells. In longer 7 day-co-cultures, LY-411575 minimally affected BCMAxCD3 BisAb (PL33)-induced transient expression of checkpoint (PD1, TIGIT, TIM3, LAG3) and co-stimulatory (41BB, CD28) proteins, as well as time-dependent increases in % effector memory/central memory subsets and CD8/CD4 ratios in patient T cells. Importantly, LY41157 rapidly cleared sBCMA from circulation of MM-bearing NSG mice reconstituted with human T cells and significantly enhanced anti-MM efficacy of PL33 with prolonged host survival. Taken together, these results further support ongoing combination BCMA-targeting immunotherapies with GSI clinical studies to improve patient outcome.

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Publisher

Springer Nature B.V

Subject

Antibodies

/ Antigens

/ Biomedical research

/ Cancer therapies

/ Cloning

/ Cytotoxicity

/ Drug dosages