HGG-20. CANCER PREDISPOSITION SYNDROMES IN PEDIATRIC PATIENTS WITH HIGH-GRADE GLIOMAS

Abstract

Abstract The association between pediatric high-grade gliomas (HGG) and cancer predisposition syndromes (CPS) remains inadequately elucidated in the existing literature, while next-generation sequencing (NGS) is increasingly utilized for diagnostic support. In this retrospective analysis, we evaluated a cohort of 95 consecutive pediatric patients with HGG reclassified according to the latest 2021 WHO classification, diagnosed and treated at the Bambino Gesù Children’s Hospital between 2011 and 2023. All patients underwent genetic germline testing with NGS technology to detect the presence of germline variants predisposing to cancer and were included in this study. Diagnosis of pHGG H3-IDH wild-type was performed in 23 patients (24.2%), diffuse midline glioma in 46 patients (48.4%), astrocytoma IDH-mutant in 7 patients (7.4%), anaplastic pleomorphic xanthoastrocytoma in 4 patients (4.2%), adult type HGG in 4 patients (4.2%), neuroepithelial tumor PATZ1 fusion-positive in 3 patients (3.2%), diffuse hemispheric glioma H3 G34-mutant in 2 patients (2.1%), infant-type hemisheric glioma in 2 patients (2.1%), other rare histologies in 4 patients (4.2%). Oncological family history was investigated up to the third generation for all patients and was positive in 43/95 (45.3%) cases. We identified a total of 65 variants in 95 patients, distributed as follows: 48 variants of uncertain significance (73.8%), 10 likely pathogenic (15.4%), and 7 pathogenic variants (10.8%). Notably, our findings reveal that pathogenic/likely pathogenic variants were detected in about 17% of the entire study population, higher than the 10% incidence reported in the existing literature. The high rate of mutations in CPS associated genes described in our work, leads to consider performing NGS even in the absence of clinical or anamnestic criteria suggestive of it. However, ethical and social issues are to be considered when we propose and investigate patients for CPS. Moreover, further research are needed to determine the role of variants of uncertain significance.