DIPG-76. PEDIATRIC PATIENTS WITH DIFFUSE MIDLINE GLIOMA DEMONSTRATE AN UNEXPECTED PREVALENCE OF GERMLINE VARIANTS IN HOMOLOGOUS RECOMBINATION GENES

Marion K Mateos,Marion K Mateos,Ann Altekoester,Chris Jones,Katherine Tucker,Kimberly Dias,Mirjam Blattner-Johnson,Catherine Goudie,Elisha Hayden,Chelsea Mayoh,Alison Salkeld,Orazio Vittorio,Nikoleta Juretic,Mark J Cowley,Elke Pfaff,Jo Lynne Rokita,Sebastian M Waszak,Elke Pfaff,Chelsea Mayoh,Alan Mackay,David S Ziegler,Loretta M S Lau,Holly Holiday,Sebastien Perreault,Stefan M Pfister,Jo Lynne Rokita,Stefan M Pfister,Paulette Barahona,Katherine Tucker,Mark Pinese,Maria Tsoli,Adam Resnick,Sabine Mueller,Alison Salkeld,Paulette Barahona,Christof M Kramm,Adam Resnick,Louise Cui,Dong-Anh Khuong-Quang,Yiran Guo,Holly Holiday,Maria Tsoli,Nada Jabado,Mark Pinese,Sam El Kamand,Marie Wong-Erasmus,Orazio Vittorio,Jie Liu,Loretta M S Lau,Mark J Cowley,David T W Jones,Catherine Goudie,Noemi Fuentes-Bolanos,Sebastian M Waszak,David S Ziegler,Noemi Fuentes-Bolanos,Pamela Ajuyah,Dong-Anh Khuong-Quang

doi:10.1093/neuonc/noae064.129

Abstract

Abstract BACKGROUND Pediatric patients with Diffuse Midline Gliomas (DMG), H3K27M altered have a dismal prognosis and novel therapeutic approaches are urgently needed. Factors that drive development of pediatric DMG are unknown. METHODS To determine the prevalence of germline pathogenic/likely pathogenic variants (P/LPV) in DMG, we assembled an international cohort of 252 patients with germline whole genome or whole exome sequencing data, including diffuse intrinsic pontine glioma (DIPG; n=153), from Australian, European and North American centres. RESULTS We identified germline P/LPV in cancer predisposition genes in 7.5% (19/252) of patients, mainly homologous recombination (n=9; BRCA1, BRCA2, PALB2) and Fanconi anemia genes (n=4). Germline P/LPV in mismatch repair genes (MSH2, PMS2) were found in two patients. Two patients each had two separate germline P/LPV. The prevalence of germline P/LPV was not significantly different according to age, location of DMG nor H3K27M mutational status. Furthermore, tumor profiles differed, with absence of somatic drivers in the PI3K/mTOR pathway in patients with germline P/LPV compared to those without (P = 0.023). Knockdown of BRCA1 in DMG cell cultures sensitized tumor cells to PARP inhibition. Reflecting the potential therapeutic relevance of these findings, we describe one H3.3 K27M-mutant DMG patient with a pathogenic germline BRCA2 and FANCE variant and multiple recurrences, who was treated with a PARP inhibitor (olaparib) and immune checkpoint inhibitor, leading to a near complete radiological response after 4 months. CONCLUSION Our study is the largest series to date investigating germline P/LPV in cancer predisposition genes in DMG and provides new therapeutic insights. It is expected that these germline findings will also guide cascade testing for a proband’s relatives. Our data highlight the importance of germline testing in H3K27-altered DMG patients at diagnosis.

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