Intravenous and intracranial GD2-CAR T cells for H3K27M+ diffuse midline gliomas

Michelle Monje(Howard Hughes Medical Institute), Jasia Mahdi(Stanford University), Robbie G. Majzner(Stanford University), Kristen W. Yeom(Stanford University), Liora M. Schultz(Stanford University), Rebecca M. Richards(Stanford University), Valentin Barsan(Stanford University), Kun-Wei Song(Stanford University), Jen Kamens(Stanford University), Christina Baggott(Stanford University), Michael Kunicki(Stanford University), Skyler P. Rietberg(Stanford University), Alexandria Sung Lim(Stanford University), Agnes Reschke(Stanford University), Sharon Mavroukakis(Stanford University), Emily Egeler(Stanford University), Jennifer Moon(Stanford University), Shabnum Patel(Stanford University), Harshini Chinnasamy(Stanford University), Courtney Erickson(Stanford University), Ashley Jacobs(Stanford University), Allison K. Duh(Stanford University), Ramya Tunuguntla(Stanford University), Dorota D. Klysz(Stanford University), Carley Fowler(Stanford University), Sean Green(Stanford University), Barbara Beebe(Stanford University), Casey Carr(Stanford University), Michelle Fujimoto(Stanford University), Annie Kathleen Brown(Stanford University), Ann-Louise G. Petersen(Stanford University), Catherine McIntyre(Stanford Health Care), Aman Siddiqui(Stanford Health Care), Nadia Lepori‐Bui(Stanford Health Care), Katlin Villar(Stanford Health Care), Kymhuynh Pham(Stanford Health Care), Rachel Bove(Stanford Health Care), Eric Musa(Stanford Health Care), Warren D. Reynolds(Stanford University), Adam Kuo(Stanford University), Snehit Prabhu(Stanford University), Lindsey Rasmussen(Stanford University), Timothy T. Cornell(Stanford University), Sonia Partap(Stanford University), Paul G. Fisher(Stanford University), Cynthia Campen(Stanford University), Gerald A. Grant(Stanford University), Laura M. Prolo(Stanford University), Xiaobu Ye(Johns Hopkins University), Bita Sahaf(Stanford University), Kara L. Davis(Stanford University), Steven A. Feldman(Stanford University), Sneha Ramakrishna(Stanford Medicine), Crystal L. Mackall(Parker Institute for Cancer Immunotherapy)
Nature
November 13, 2024
Cited by 160Open Access
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Abstract

Abstract H3K27M-mutant diffuse midline gliomas (DMGs) express high levels of the disialoganglioside GD2 (ref. 1 ). Chimeric antigen receptor-modified T cells targeting GD2 (GD2-CART) eradicated DMGs in preclinical models 1 . Arm A of Phase I trial no. NCT04196413 (ref. 2 ) administered one intravenous (IV) dose of autologous GD2-CART to patients with H3K27M-mutant pontine (DIPG) or spinal DMG (sDMG) at two dose levels (DL1, 1 × 10 6 kg − 1 ; DL2, 3 × 10 6 kg −1 ) following lymphodepleting chemotherapy. Patients with clinical or imaging benefit were eligible for subsequent intracerebroventricular (ICV) intracranial infusions (10–30 × 10 6 GD2-CART). Primary objectives were manufacturing feasibility, tolerability and the identification of maximally tolerated IV dose. Secondary objectives included preliminary assessments of benefit. Thirteen patients enroled, with 11 receiving IV GD2-CART on study ( n = 3 DL1 (3 DIPG); n = 8 DL2 (6 DIPG, 2 sDMG)). GD2-CART manufacture was successful for all patients. No dose-limiting toxicities occurred on DL1, but three patients experienced dose-limiting cytokine release syndrome on DL2, establishing DL1 as the maximally tolerated IV dose. Nine patients received ICV infusions, with no dose-limiting toxicities. All patients exhibited tumour inflammation-associated neurotoxicity, safely managed with intensive monitoring and care. Four patients demonstrated major volumetric tumour reductions (52, 54, 91 and 100%), with a further three patients exhibiting smaller reductions. One patient exhibited a complete response ongoing for over 30 months since enrolment. Nine patients demonstrated neurological benefit, as measured by a protocol-directed clinical improvement score. Sequential IV, followed by ICV GD2-CART, induced tumour regressions and neurological improvements in patients with DIPG and those with sDMG.


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