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. 2022 Nov 14;24(Suppl 7):vii86–vii87. doi: 10.1093/neuonc/noac209.326

CTNI-61. CLINICAL EFFICACY AND PREDICTIVE BIOMARKERS OF ONC201 IN H3K27M-MUTANT DIFFUSE MIDLINE GLIOMA

Abed Rahman Kawakibi 1, Rohinton Tarapore 2, Sharon Gardner 3, Andrew Chi 4, Sylvia Kurz 5, Patrick Y Wen 6, Isabel Arrillaga-Romany 7, Tracy Batchelor 8, Nicholas Butowski 9, Ashley Sumrall 10, Nicole Shonka 11, Rebecca Harrison 12, John DeGroot 13, Minesh Mehta 14, Yazmin Odia 15, Matthew Hall 16, Doured Daghistani 17, Timothy Cloughesy 18, Benjamin Ellingson 19, Michelle Kim 20, Yoshie Umemura 21, Hugh Garton 22, Andrea Franson 23, Jonathan Schwartz 24, Sunjong Li 25, Rodrigo Cartaxo 26, Karthik Ravi 27, Evan Cantor 28, Jessica Cummings 29, Alyssa Paul 30, Dustin Walling 31, Matthew Dun 32, Jason Cain 33, Jiang Li 34, Mariella Filbin 35, Lili Zhao 36, Chandan Kumar-Sinha 37, Rajen Mody 38, Arul Chinnaiyan 39, Ryo Kurokawa 40, Drew Pratt 41, Sriram Venneti 42, Jacques Grill 43, Cassie Kline 44, Sabine Mueller 45, Adam C Resnick 46, Javad Nazarian 47, Sebastian Waszak 48, Joshua E Allen 49, Carl Koschmann 50
PMCID: PMC9660897

Abstract

Patients with H3K27M-mutated diffuse midline glioma (DMG) have no proven effective therapies beyond radiation. ONC201, a DRD2 antagonist and mitochondrial ClpP agonist, has shown promise in this population. Clinical and genetic variables associated with ONC201 response in H3K27M-mutant DMG continue to be investigated. A combined clinical and genetic study evaluated patients with H3K27M-DMG treated with single-agent ONC201 at the established phase 2 dose. Clinical outcomes of patients treated on two recently completed multi-site clinical studies (NCT03416530 and NCT03134131, n = 75) were compared with historical control data from patients with confirmed H3K27M-DMG (n = 391 total, n = 119 recurrent). Patients treated with ONC201 monotherapy following initial radiation, but prior to recurrence, demonstrated a median overall survival (OS) of 25.6 months from diagnosis and recurrent patients demonstrated a median OS of 16.2 months from recurrence, both of these more than doubling historical outcomes. Using a Cox model to correct for age, gender and tumor location, OS of ONC201-treated patients with H3K27M-mutant tumors remained significantly better than non-ONC201-treated historical controls (p = 0.0001). A survival and radiographic analysis based on tumor location, revealed stronger responses in thalamic patients. In patients with thalamic tumors treated after initial radiation (n = 16), median OS was not reached with median follow up of 22.1 months (historical control median OS of 12.5 months, n = 83, p = 0.0001). Significant correlations were found between baseline cerebral blood flow (CBF) on perfusion imaging and OS (Pearson’s r = 0.75, p = 0.003) and between nrCBF and PFS (r = 0.77, p = 0.002). Baseline tumor sequencing from treated patients (n = 20) demonstrates EGFR mutation (n = 3) and high EGFR expression as a marker of resistance and improved response in tumors with MAPK-pathway alterations (n = 5). In conclusion, ONC201 demonstrates unprecedented clinical and radiographic efficacy in H3K27M-mutant DMG with outcomes enriched in patients with thalamic tumors, treatment prior to recurrence, MAPK-pathway alterations, and patients with relatively high CBF.

Articles from Neuro-Oncology are provided here courtesy of Society for Neuro-Oncology and Oxford University Press

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