Mesothelin is a surface antigen present on human meningioma and can be effectively targeted by CAR T-cells.

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作者:Ramapriyan Rishab, Barker Fred G 2nd, Richardson Leland G, Sun Jing, Vandecandelaere Gust, Shim Jane M, De Vlaminck Guillaume, Gaffey Matthew, Grewal Eric P, Tazhibi Masih, Morshedy Kourosh, Aref Amir R, Batool Syeda M, Guo Xiaopeng, Ijad Nazanin, Balaj Leonora, Wakimoto Hiroaki, Martinez-Lage Maria, Frigault Matthew J, Leick Mark B, Bernstock Joshua D, Bi Wenya Linda, Carter Bob S, Chiocca E Antonio, Dietrich Jorg, Gerstner Elizabeth R, Boland Genevieve M, Nahed Brian V, Plotkin Scott R, Jenkins Russell W, Brastianos Priscilla K, Curry William T, Maus Marcela V, Choi Bryan D
BACKGROUND: Meningioma is the most common primary CNS tumor, with high-grade cases exhibiting aggressive behavior, frequent recurrence, and poor prognosis. Currently, no systemic therapies are approved for recurrent or malignant meningiomas. Chimeric antigen receptor (CAR) T-cell therapy has shown efficacy in hematologic malignancies and promise for solid tumors, but its use for meningiomas has been underexplored. Mesothelin, a glycoprotein overexpressed in several solid tumors of mesodermal origin, may serve as a viable immunotherapeutic target. This study aimed to evaluate mesothelin as a CAR T-cell target in meningiomas. METHODS: Mesothelin expression was analyzed in patient-derived meningioma samples using immunohistochemistry, flow cytometry, and droplet digital PCR. Mesothelin-specific CAR T-cells were generated and evaluated invitro, exvivo using patient-derived organotypic tumor spheroids (PDOTS), and invivo using orthotopic meningioma mouse models of human xenografts. Cytotoxicity, T-cell proliferation, cytokine secretion, and tumor clearance were assessed. RESULTS: Mesothelin was detected in a subset of tumors across all meningioma grades at the transcript and protein levels, with surface expression confirmed in patient-derived primary cells. Mesothelin-specific CAR T-cells exhibited potent and specific cytotoxicity, T-cell activation, and cytokine secretion in vitro and effectively eliminated PDOTS. In orthotopic human xenograft models, mesothelin CAR T-cell therapy led to significant tumor regression and prolonged survival. CONCLUSIONS: Mesothelin is a viable CAR T-cell target for meningiomas, and mesothelin-specific CAR T-cell therapy shows strong preclinical efficacy. These findings provide a rationale for early-phase clinical trials of mesothelin CAR T-cell therapy in patients with refractory meningiomas.

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