CERN 09-02: A PHASE 2 TRIAL OF CARBOPLATIN AND BEVACIZUMAB FOR RECURRENT ADULT EPENDYMOMA

Authors

• Shuodan Zhang
• Byram Ozer
• Antonio Omuro
• Ying Yuan
• Tito Mendoza
• Kathleen Wall
• Eva Grajkowska
• Elizabeth Vera
• Jennifer Reyes
• Kenneth Aldape
• Jing Wu
• Marta Penas-Prado
• Eric Burton
• Tobias Walbert, Henry Ford HealthFollow
• Tom Mikkelsen, Henry Ford HealthFollow
• Shiao-Pei Weathers
• Barbara O’Brien
• John de Groot
• Vinay Puduvalli
• Lisa DeAngelis
• Thomas J. Kaley
• Elena Pentsova
• Igor Gavrilovic
• Elizabeth Gerstner
• Terri Armstrong
• Mark Gilbert

Recommended Citation

Zhang S, Ozer B, Omuro A, Yuan Y, Mendoza T, Wall K, Grajkowska E, Vera E, Reyes J, Aldape K, Wu J, Penas-Prado M, Burton E, Walbert T, Mikkelsen T, Weathers S, O’Brien B, de Groot J, Puduvalli V, DeAngelis L, Kaley TJ, Pentsova E, Gavrilovic I, Gerstner E, Armstrong T, Gilbert M. CERN 09-02: A PHASE 2 TRIAL OF CARBOPLATIN AND BEVACIZUMAB FOR RECURRENT ADULT EPENDYMOMA. Neuro Oncol 2025; 27:v142.

Document Type

Conference Proceeding

Publication Date

11-11-2025

Publication Title

Neuro Oncol

Keywords

bevacizumab, carboplatin, adult, brain disease, brain tumor, clinical article, cognition, conference abstract, drug therapy, ependymoma, female, follow up, human, male, multiple cycle treatment, patient-reported outcome, phase 2 clinical trial, progression free survival, questionnaire, salvage therapy, side effect, spinal cord disease, survival rate, symptom burden

Abstract

BACKGROUND: Salvage therapies for adults with recurrent ependymoma are limited. A prior retrospective review of patients with recurrent ependymoma treated with bevacizumab and carboplatin reported a 75% radiographic response rate. This prospective single arm, open label Phase 2 study was designed to confirm these results. METHODS: 22 patients were evaluated in this CERN Adult Clinical Trials network study. Adult patients (age ≥ 18) with recurrent ependymoma were treated with both carboplatin (AUC = 5 -6) every 4 weeks and bevacizumab 10mg/kg every 2 weeks for 6 cycles, after which carboplatin was discontinued, and bevacizumab could be continued at physician's discretion. Imaging of areas involved by tumor, and patient reported outcomes with the MD Anderson Symptom Inventory questionnaires (brain and/or spine modules) were assessed at baseline and every 2 cycles to evaluate response and symptom burden, respectively. RESULTS: With a median follow-up time of 25.9 months, the primary end point of 12-month progression free survival rate (PFS-12) greater than 50% was reached with a rate of 76.4% (95% CI, 52.2, 89.4). The median PFS of this cohort was 18.0 months. Two patients achieved a partial response (9.1%). There were no treatment-related grade 4 toxicities. Improved cognitive and neurological symptoms were observed in brain tumor responders, while spine tumor patients had worsening symptom outcomes regardless of response. CONCLUSIONS: Treatment with carboplatin and bevacizumab in adult recurrent ependymoma reached the PFS-12 clinical efficacy threshold, suggesting that this treatment has efficacy in this patient population. However, symptomatic worsening in patients with spinal cord disease does raise concerns that bevacizumab pseudoresponse may account for some imaging stability and symptom improvement with brain disease.

Volume

27

First Page

v142