Sexually dimorphic radiogenomic models identify distinct imaging and biological pathways that are prognostic of overall survival in glioblastoma

Abstract Background Recent epidemiological studies have suggested that sexual dimorphism influences treatment response and prognostic outcome in glioblastoma (GBM). To this end, we sought to (i) identify distinct sex-specific radiomic phenotypes—from tumor subcompartments (peritumoral edema, enhanci...

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Veröffentlicht in:Neuro-oncology (Charlottesville, Va.) Va.), 2021-02, Vol.23 (2), p.251-263
Hauptverfasser: Beig, Niha, Singh, Salendra, Bera, Kaustav, Prasanna, Prateek, Singh, Gagandeep, Chen, Jonathan, Saeed Bamashmos, Anas, Barnett, Addison, Hunter, Kyle, Statsevych, Volodymyr, Hill, Virginia B, Varadan, Vinay, Madabhushi, Anant, Ahluwalia, Manmeet S, Tiwari, Pallavi
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Sprache:eng
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Zusammenfassung:Abstract Background Recent epidemiological studies have suggested that sexual dimorphism influences treatment response and prognostic outcome in glioblastoma (GBM). To this end, we sought to (i) identify distinct sex-specific radiomic phenotypes—from tumor subcompartments (peritumoral edema, enhancing tumor, and necrotic core) using pretreatment MRI scans—that are prognostic of overall survival (OS) in GBMs, and (ii) investigate radiogenomic associations of the MRI-based phenotypes with corresponding transcriptomic data, to identify the signaling pathways that drive sex-specific tumor biology and treatment response in GBM. Methods In a retrospective setting, 313 GBM patients (male = 196, female = 117) were curated from multiple institutions for radiomic analysis, where 130 were used for training and independently validated on a cohort of 183 patients. For the radiogenomic analysis, 147 GBM patients (male = 94, female = 53) were used, with 125 patients in training and 22 cases for independent validation. Results Cox regression models of radiomic features from gadolinium T1-weighted MRI allowed for developing more precise prognostic models, when trained separately on male and female cohorts. Our radiogenomic analysis revealed higher expression of Laws energy features that capture spots and ripple-like patterns (representative of increased heterogeneity) from the enhancing tumor region, as well as aggressive biological processes of cell adhesion and angiogenesis to be more enriched in the “high-risk” group of poor OS in the male population. In contrast, higher expressions of Laws energy features (which detect levels and edges) from the necrotic core with significant involvement of immune related signaling pathways was observed in the “low-risk” group of the female population. Conclusions Sexually dimorphic radiogenomic models could help risk-stratify GBM patients for personalized treatment decisions.
ISSN:1522-8517
1523-5866
DOI:10.1093/neuonc/noaa231