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Merck

GD2 CAR T cells against human glioblastoma.

NPJ precision oncology (2021-10-29)
Malvina Prapa, Chiara Chiavelli, Giulia Golinelli, Giulia Grisendi, Marco Bestagno, Rosanna Di Tinco, Massimiliano Dall'Ora, Giovanni Neri, Olivia Candini, Carlotta Spano, Tiziana Petrachi, Laura Bertoni, Gianluca Carnevale, Giuseppe Pugliese, Roberta Depenni, Alberto Feletti, Corrado Iaccarino, Giacomo Pavesi, Massimo Dominici
RESUMEN

Glioblastoma is the most malignant primary brain tumor and is still in need of effective medical treatment. We isolated patient-derived glioblastoma cells showing high GD2 antigen expression representing a potential target for CAR T strategy. Data highlighted a robust GD2 CAR antitumor potential in 2D and 3D glioblastoma models associated with a significant and CAR T-restricted increase of selected cytokines. Interestingly, immunosuppressant TGF β1, expressed in all co-cultures, did not influence antitumor activity. The orthotopic NOD/SCID models using primary glioblastoma cells reproduced human histopathological features. Considering still-conflicting data on the delivery route for targeting brain tumors, we compared intracerebral versus intravenous CAR T injections. We report that the intracerebral route significantly increased the length of survival time in a dose-dependent manner, without any side effects. Collectively, the proposed anti-GD2 CAR can counteract human glioblastoma potentially opening a new therapeutic option for a still incurable cancer.

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Sigma-Aldrich
Proteinasa K from Tritirachium album, lyophilized powder, BioUltra, ≥30 units/mg protein, for molecular biology
Sigma-Aldrich
Anticuerpo anti-mitocondrial, superficie de mitocondrias intactas, clon 113-1, clone 113-1, Chemicon®, from mouse
Sigma-Aldrich
Lectina de Phaseolus vulgaris (frijol rojo), Erythroagglutinin PHA-E