Abstract Details

Title Integrating Molecular Profiling into Glioma Diagnosis: Implications of the WHO-CNS5-2021 Classification

Topic Neuro-oncology

Presentation(s) P4 - Poster Session 4 (5:00 PM-6:00 PM)

Poster/Presentation
Number 6-008

Objective We aimed to conduct a comprehensive molecular characterization of gliomas following the WHO-CNS5-2021 classification and to compare it with histopathological evaluations.

Background Gliomas are the most frequent primary malignant brain tumors. The current classification includes histopathologic features and molecular biomarkers with defined roles in pathogenesis, therapeutics, and prognosis. Adopting these translational methods in clinical practice represents an educational, clinical, and resource challenge that may hinder its implementation. Understanding how this paradigm shift might change previous histopathological diagnoses could improve adherence to molecular diagnosis practices.

Design/Methods

We conducted a descriptive study. We analyzed glioma DNA using Sanger sequencing, multiplex ligation-dependent probe amplification (MLPA), and methylation-specific MLPA (MS-MLPA). We assessed mutations in IDH1, IDH2, TERT, EGFR amplification, homozygous CDKN2A deletion, 1p/19q codeletion and the methylation status of the MGMT promoter.

Results We included 22 Colombian patients, 41% of whom were male. Glioblastoma was the most frequent histopathological diagnosis (68.2%, n=15), followed by astrocytoma (9%, n=2) and oligodendroglioma (4.5%, n =1). After molecular characterization, most patients were identified as IDH-wildtype (59% n=13) and were classified as glioblastoma IDH-Wildtype WHO grade 4. We identified non-canonical IDH1 mutations (p.R132S) in 14% (n=3) samples. MGMT promoter was hyper-methylated in 40% of the glioblastomas IDH-wildtype. The discordance rate between histopathological and molecular diagnosis was 21%, primarily due to tumors initially described as glioblastomas being reclassified as astrocytomas IDH-mutant.

Conclusions Our findings highlight the critical importance of integrating molecular profiling into diagnostic workflow for gliomas. One out of five gliomas were reclassified with a more benign phenotype using the WHO-CNS5-2021 molecular classification. This discrepancy underscores the limitations of traditional methods and emphasizes the need for routine molecular assessment to ensure accurate diagnosis. A broader adoption of molecular diagnosis might enhance diagnosis precision and therapeutic strategies. Further molecular profiling is needed to refine classification systems and identify new biomarkers.

Authors/Disclosures
Andrés F. Patiño-Aldana, MD, MSc PRESENTER	Dr. Patiño-Aldana has nothing to disclose.
Omar Echeverria Gomez, MD	Mr. Echeverria Gomez has nothing to disclose.
Ana M. Chinchilla Rendón, Student	Miss Chinchilla Rendón has nothing to disclose.
Nora Contreras, Master	Miss Contreras has nothing to disclose.
Camilo S. Peralta Rache, Bsc	Mr. Peralta Rache has nothing to disclose.
Nicolas A. Caballero, MD	Dr. Caballero has nothing to disclose.
Hanna V. Tovar-Romero, MD	Dr. Tovar-Romero has nothing to disclose.
Jose M. Palacio, Sr., MD	Mr. Palacio has nothing to disclose.
Veronica Uribe Andrade, MD, Estudiante de Medicina	Miss Uribe Andrade has nothing to disclose.
Matteo Mineo, Student	Mr. Mineo has nothing to disclose.
fernando A. velandia, Sr.	Prof. velandia has nothing to disclose.
Daniel F. Silgado Guzmán, Sr., MSc	Mr. Silgado Guzmán has nothing to disclose.
William M. Riveros, Sr., MD	Dr. Riveros has nothing to disclose.
Alejandro O. Ondo-Méndez, PhD	Prof. Ondo-Méndez has nothing to disclose.
Dora Fonseca	Prof. Fonseca has nothing to disclose.

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