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CAR-T cells secreting BiTEs circumvent antigen escape without detectable toxicity. 2019
Bryan D Choi, and
Xiaoling Yu, and
Ana P Castano, and
Amanda A Bouffard, and
Andrea Schmidts, and
Rebecca C Larson, and
Stefanie R Bailey, and
Angela C Boroughs, and
Matthew J Frigault, and
Mark B Leick, and
Irene Scarfò, and
Curtis L Cetrulo, and
Shadmehr Demehri, and
Brian V Nahed, and
Daniel P Cahill, and
Hiroaki Wakimoto, and
William T Curry, and
Bob S Carter, and
Marcela V Maus
Cellular Immunotherapy Program, Cancer Center, Massachusetts General Hospital and Harvard Medical School, Boston, MA, USA.
Chimeric antigen receptor (CAR)-T-cell therapy for solid tumors is limited due to heterogeneous target antigen expression and outgrowth of tumors lacking the antigen targeted by CAR-T cells directed against single antigens. Here, we developed a bicistronic construct to drive expression of a CAR specific for EGFRvIII, a glioblastoma-specific tumor antigen, and a bispecific T-cell engager (BiTE) against EGFR, an antigen frequently overexpressed in glioblastoma but also expressed in normal tissues. CART.BiTE cells secreted EGFR-specific BiTEs that redirect CAR-T cells and recruit untransduced bystander T cells against wild-type EGFR. EGFRvIII-specific CAR-T cells were unable to completely treat tumors with heterogenous EGFRvIII expression, leading to outgrowth of EGFRvIII-negative, EGFR-positive glioblastoma. However, CART.BiTE cells eliminated heterogenous tumors in mouse models of glioblastoma. BiTE-EGFR was locally effective but was not detected systemically after intracranial delivery of CART.BiTE cells. Unlike EGFR-specific CAR-T cells, CART.BiTE cells did not result in toxicity against human skin grafts in vivo.
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