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Using the Epitranscriptome to Diagnose and Treat Gliomas

Status: Recruiting
Location: See all (2) locations...
Intervention Type: Diagnostic test
Study Type: Interventional
Study Phase: Not Applicable
SUMMARY

Diffuse gliomas are among the most common tumors of the central nervous system, with high morbidity and mortality and very limited therapeutic possibilities. The diffuse glioma are characterized by significant variability in terms of age at diagnosis, histological and molecular features, classification, ability to transform to a higher grade and/or to disseminate in the brain, response to treatment and patient outcome. One of the main challenges in the management of diffuse gliomas is related to tumor heterogeneity within the same subgroup. Establishing an accurate tumor classification is of paramount importance for selecting personalized therapy or avoiding unnecessary treatment. At present, the main diagnostic methods for detecting gliomas are based on histopathological features and mutation detection. Yet difficulties remain, due to tumor heterogeneity and sampling bias for tumors obtained from small biopsies. In particular, grade 2 (low-grade) and grade 3 (high-grade) gliomas cannot be easily distinguished, as intra-tumoral tumor grade heterogeneity is not uncommon in patients treated with extensive surgical resection. Another challenge in the field of gliomas is longitudinal monitoring of disease progression, which is currently mainly based on repeated brain Magnetic Resonance Imaging (MRI). New tools to detect tumor changes before the onset of imaging changes would be useful. Several genetic, epigenetic, metabolic and immunological profiles have been established for gliomas. Recently, the world of RiboNucleic Acid (RNA) has emerged as a promising area to explore for cancer therapy, especially since the (re)discovery of RNA chemical modifications. To date, more than 150 types of post-transcriptional modifications have been reported on various RNA molecules. This complex landscape of chemical marks embodies a new, invisible code that governs the post-transcriptional fate of RNA: stability, splicing, storage, translation.

Eligibility
Participation Requirements
Sex: All
Minimum Age: 18
Healthy Volunteers: t
View:

• Male / female over 18 years of age,

• Surgery (tumor resection) scheduled at Montpellier University Hospital for suspected, diffuse glioma, confirmed on tissue sample: IDH mutated grade 2 glioma (excluding tumors with a focus of grade 3 or 4 glioma), IDH mutated grade 3 glioma or GBM, IDH wild-type,

• No history of treatment (surgery, radiotherapy or chemotherapy) for glioma,

• Willingness and ability to comply with scheduled visits, treatment plan, laboratory tests and other study procedures,

• Patient has given express written informed consent prior to any study procedure,

• Patient affiliated to a French health insurance.

Locations
Other Locations
France
CHU Montpellier - Hôpital St Eloi
RECRUITING
Montpellier
Insitut Régional du Cancer de Montpellier
RECRUITING
Montpellier
Contact Information
Primary
Aurore MOUSSION
aurore.moussion@icm.unicancer.fr
467612446
Backup
Emmanuelle TEXIER
emmanuelle.texier@icm.unicancer.fr
467613102
Time Frame
Start Date: 2026-06-01
Estimated Completion Date: 2031-05
Participants
Target number of participants: 228
Treatments
Other: Cohort 1
Prospective cohort: 80 patients and 20 healthy volunteers~* Grade 2 mutated Isocitrate Dehydrogenase (IDH) glioma: 20 patients~* IDH mutated grade 3 glioma: 20 patients~* Glioblastoma (GBM), IDH wild-type: 40 patients
Other: Cohort 2
Retrospective cohort: 120 patients~* Grade 2 mutated Isocitrate Dehydrogenase (IDH) glioma: 40 patients~* IDH mutated grade 3 glioma: 40 patients~* Glioblastoma, IDH wild-type: 40 patients
Other: Cohort 3
Spatial epitranscriptomic cohort: 8 patients (grade 2 mutated Isocitrate Dehydrogenase (IDH ) glioma with grade 3 or grade 4 focus
Related Therapeutic Areas
Sponsors
Leads: Institut du Cancer de Montpellier - Val d'Aurelle
Collaborators: National Cancer Institute, France

This content was sourced from clinicaltrials.gov