Dual targeting ovarian cancer by Muc16 CAR T cells secreting a bispecific T cell engager antibody for an intracellular tumor antigen WT1

被引:0
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作者
Sung Soo Mun
Jeremy Meyerberg
Leila Peraro
Tatyana Korontsvit
Thomas Gardner
Manish Malviya
Chrisann Kyi
Roisin E. O’Cearbhaill
Cheng Liu
Tao Dao
David A. Scheinberg
机构
[1] Memorial Sloan Kettering Cancer Center,Molecular Pharmacology Program
[2] Memorial Sloan Kettering Cancer Center,Gynecologic Medical Oncology Service, Department of Medicine
[3] Weill Cornell Medical College,undefined
[4] Eureka Therapeutics,undefined
[5] Inc.,undefined
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关键词
Dual targeting; Muc16 CAR T cells; TCR mimic mAb; WT1; ESK1 BiTE;
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摘要
Epithelial ovarian cancer is the most lethal of gynecological cancers. The therapeutic efficacy of chimeric antigen receptor (CAR) T cell directed against single antigens is limited by the heterogeneous target antigen expression in epithelial ovarian tumors. To overcome this limitation, we describe an engineered cell with both dual targeting and orthogonal cytotoxic modalities directed against two tumor antigens that are highly expressed on ovarian cancer cells: cell surface Muc16 and intracellular WT1. Muc16-specific CAR T cells (4H11) were engineered to secrete a bispecific T cell engager (BiTE) constructed from a TCR mimic antibody (ESK1) reactive with the WT1-derived epitope RMFPNAPYL (RMF) presented by HLA-A2 molecules. The secreted ESK1 BiTE recruited and redirected other T cells to WT1 on the tumor cells. We show that ESK1 BiTE-secreting 4H11 CAR T cells exhibited enhanced anticancer activity against cancer cells with low Muc16 expression, compared to 4H11 CAR T cells alone, both in vitro and in mouse tumor models. Dual orthogonal cytotoxic modalities with different specificities targeting both surface and intracellular tumor-associated antigens present a promising strategy to overcome resistance to CAR T cell therapy in epithelial ovarian cancer and other cancers.
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页码:3773 / 3786
页数:13
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