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P32-specific CAR T cells with dual antitumor and antiangiogenic therapeutic potential in gliomas

by Waks, Tova , Friedmann-Morvinski, Dinorah , Teesalu, Tambet , Rousso-Noori, Liat , Talmor, Shauli , Globerson Levin, Anat , Mastandrea, Ignacio , Haugas, Maarja , Alvarez-Vallina, Luis , Eshhar, Zelig

in 13 / 13/106 / 13/31 / 13/51 / 14/19 / 42 / 42/44 / 59 / 59/5 / 631/67/1059/2325 / 631/67/1922 / 64/60 / 692/4028/67/1922 / Animal models / Antiangiogenics / Antigens / Cell culture / Cell therapy / Chimeric antigen receptors / Endothelial cells / Feasibility studies / Glioblastoma / Glioma / Glioma cells / Heterogeneity / Humanities and Social Sciences / Lymphocytes / Lymphocytes T / multidisciplinary / Patients / Receptors / Science / Science (multidisciplinary) / Tumors / Xenografts / Xenotransplantation

2021

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P32-specific CAR T cells with dual antitumor and antiangiogenic therapeutic potential in gliomas

2021

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P32-specific CAR T cells with dual antitumor and antiangiogenic therapeutic potential in gliomas

2021

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Journal Article

P32-specific CAR T cells with dual antitumor and antiangiogenic therapeutic potential in gliomas

Waks, Tova,

Friedmann-Morvinski, Dinorah,

Teesalu, Tambet,

Rousso-Noori, Liat,

Talmor, Shauli,

Globerson Levin, Anat,

Mastandrea, Ignacio,

Haugas, Maarja,

Alvarez-Vallina, Luis,

Eshhar, Zelig

2021

Overview

Glioblastoma is considered one of the most aggressive malignancies in adult and pediatric patients. Despite decades of research no curative treatment is available and it thus remains associated with a very dismal prognosis. Although recent pre-clinical and clinical studies have demonstrated the feasibility of chimeric antigen receptors (CAR) T cell immunotherapeutic approach in glioblastoma, tumor heterogeneity and antigen loss remain among one of the most important challenges to be addressed. In this study, we identify p32/gC1qR/HABP/C1qBP to be specifically expressed on the surface of glioma cells, making it a suitable tumor associated antigen for redirected CAR T cell therapy. We generate p32 CAR T cells and find them to recognize and specifically eliminate p32 expressing glioma cells and tumor derived endothelial cells in vitro and to control tumor growth in orthotopic syngeneic and xenograft mouse models. Thus, p32 CAR T cells may serve as a therapeutic option for glioblastoma patients. Chimeric antigen receptor (CAR) T cell therapy has been proposed as a promising approach for treating glioblastoma. Here the authors show that p32 is expressed in murine and human glioma and that p32-directed CAR-T cells promote anti-tumor responses in preclinical models by targeting glioma cells and tumor derived endothelial cells.

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Publisher

Nature Publishing Group UK,Nature Publishing Group,Nature Portfolio

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