Abstract
BACKGROUND: Older age is often cited as a negative prognostic factor for individuals with glioblastoma, but it is unclear if this is true when other prognostic factors are equalized. METHODS: This study is an observational, single-center retrospective analysis of data from consecutive individuals with histologically identified high-grade glioma prospectively accumulated for a registry of all neurosurgical operations in our region from 2010 to 2024 (15 years). Data concerning histology, survival, IDH mutations, MGMT methylation status, extent of resection, frailty (measured by m-Fi-5 index) and subsequent adjuvant treatment (radiation and chemotherapy) were all recorded. Statistical analysis was performed on selected groups with Kaplan-Meier survival analysis, Student's t-test and multivariable Cox proportional hazards regression. RESULTS: There were 270 individuals who underwent a neurosurgical procedure resulting in a histopathological diagnosis of glioblastoma. The data from a select group of 91 individuals were examined where all individuals had tumors with IDH-wildtype, gross total resection, and treated with chemoradiation. When univariately assessing for the impact of age on survival, no significant association was found (p=0.5380). After adjusting for MGMT methylation status and frailty, age remained insignificantly associated with overall survival (p=0.4009). CONCLUSIONS: Age does not seem to be a factor in overall survival for glioblastoma when all the other prognostic factors are equalized. The idea that younger age is a positive prognostic factor is probably the result of more frequent IDH-mutant tumors in younger patients, increased incidence of frailty in older patients and the unwillingness of healthcare providers and patients/families to aggressively treat older patients.