LGG-16. PREDICTORS OF OUTCOME IN BRAF-V600E PEDIATRIC GLIOMAS TREATED WITH BRAF INHIBITORS: A REPORT FROM THE PLGG TASKFORCE

6533b829fe1ef96bd128acd8

RESEARCH PRODUCT

LGG-16. PREDICTORS OF OUTCOME IN BRAF-V600E PEDIATRIC GLIOMAS TREATED WITH BRAF INHIBITORS: A REPORT FROM THE PLGG TASKFORCE

Vijay Ramaswamy Miriam Bornhorst Murali Chintagumpala Andres Morales La Madrid Frank Van Landeghem Maria Luisa Garrè Abhi Bavle Palma Solano Bev Wilson Sarah Leary Olaf Witt Liana Nobre Jean M. Mulcahy Levy Nicholas K. Foreman Naureen Mushtaq Jack Su Jordan R. Hansford Diana S Osorio Julia Balaguer Guill David D. Eisenstat Mariana Fernandes Cornelis Vantilburg Gurcharanjeet Kaur Julie Bennett Ana Guerreiro Stucklin Valerie Larouche Sabine Mueller Till Milde Inga Harting Zdenek Pavelka Scott Ryall Eduardo Quiroga-cantero Jaroslav Sterba Josef Zamecnik Helena Mörse Michal Zapotocky Lenka Krskova Anne Grete Bechensteen Valentina Iurilli Eric Bouffet Didier Frappaz Michael D. Taylor Elisabeth Finch Adela Misove Uri Tabori Sonika Dahiya Cynthia Hawkins Alvaro Lassaletta Nisreen Amayiri Peter Hauser Tara Mckeown Ofelia Cruz Samatha Mascelli Scott L. Coven Magnus Sabel Adela Cañete Lorena Baroni Helen Toledano Roger J. Packer Sarah Injac Ute Bartels Jonathan L. Finlay David Sumerauer Cecile Faure Conter Karen Gauvain David W. Ellison Peter B. Dirks Theodore Nicolaides Duarte Salgado Daniel Alderete Matthias A. Karajannis

subject

Oncology Cancer Research medicine.medical_specialty business.industry Low Grade Glioma medicine.disease Chemotherapy regimen BRAF V600E Oncology Internal medicine Glioma Mutation (genetic algorithm)Medicine Low-Grade Glioma Neurology (clinical)business neoplasms

description

The BRAF-V600E mutation is found in 15–20% of pediatric low grade gliomas (PLGG) and result in worse outcome and higher risk of transformation to high grade gliomas (PHGG). Although ongoing trials are assessing the role of BRAF inhibitors (BRAFi) in these children, data are still limited. We aimed to report overall response rates and predictors of outcome in childhood BRAF-V600E gliomas. We collected clinical, imaging and molecular information of patients treated with BRAFi outside trials from centers participating in the PLGG taskforce. Response was calculated by RANO criteria and follow up data were collected for all patients. Sixty-six patients were treated with BRAFi (55 PLGG and 11 PHGG); median follow-up time was 1.5 years (0.1-5y). In PLGG, objective response (tumor reduction of >25%) was observed in 77% compared to 15% in a cohort treated with conventional chemotherapy (pCDKN2A deletion was not associated with lack of response, while specific enhancing patterns correlated strongly with response to BRAFi. Two-year PFS for the BRAF-V600E PLGG was 74% vs 47% for BRAFi vs chemotherapy, respectively (p=0.02). Our data reveal rapid, dramatic and sustained response of BRAF-V600E PLGG to BRAFi. These are in contrast to BRAF-V600E PHGG and non-enhancing PLGG. Additional molecular analyses are being performed to identify poor responders and emerging mechanisms of resistance in these tumors.

year	journal	country	edition	language
2019-04-01	Neuro-Oncology

https://doi.org/10.1093/neuonc/noz036.159