Fiche publication
Date publication
décembre 2025
Journal
Metabolites
Auteurs
Membres identifiés du Cancéropôle Est :
Pr NAMER Izzie-Jacques
,
Dr CEBULA Hélène
,
Dr BUND Caroline
Tous les auteurs :
Todeschi J, Cebula H, Bund C, Namer IJ
Lien Pubmed
Résumé
: High-grade glioma shows marked metabolic heterogeneity. We performed a PRISMA-guided systematic review and meta-analysis to quantify PET accuracy for pseudoprogression (PsP) and for recurrence/progression versus treatment-related change (TRC), assess pool baseline associations with overall (OS) and progression-free survival (PFS), summarize PET-based prediction of molecular markers, and assess the PET-stereotactic biopsy-ex vivo metabolomics workflow. : We searched PubMed/MEDLINE and the Web of Science Core Collection (Clarivate) from inception to 1 September 2025 for HGG cohorts with baseline PET. Eligibility: Adults with HGG; diagnostic syntheses required per-patient 2 × 2; prognostic syntheses required for HR with 95% CI. Risk of bias: QUADAS-2 (diagnostic) and QUIPS (prognostic). Random-effects models pooled log-HRs and sensitivity/specificity; molecular studies were summarized by AUCs. Imaging-to-omics concordance was reviewed narratively owing to the absence of co-registered PET-metabolite maps in human HGG. : The results included the following: OS k = 10; PFS k = 3; PsP k = 2 (N = 76); and TRC k = 3 (N = 152). For PsP, two amino acid PET cohorts yielded a sensitivity of 0.943 and a specificity of 0.826. For TRC, pooled FDOPA across two cohorts gave rise to a sensitivity of 0.879 and a specificity of 0.771. OS meta-analyses were non-significant under Hartung-Knapp modification-FDG HR of 1.09 (95% CI 0.69-1.73) and amino acid HR of 1.03 (0.72-1.46)-with substantial heterogeneity. PFS effects varied by tracer/metric; examples include FDOPA HR of 7.92 (2.17-28.90) and MET metabolic tumor volume HR of 1.60 (1.20-2.30). : Amino acid PET is sensitive to PsP and, with FDOPA, aids TRC discrimination when MRI is equivocal, whereas baseline PET-survival associations are weak and heterogeneous. Prospective co-registered PET/MR with stereotactic biopsies and HR-MAS NMR spectroscopy/MALDI-MSI is required to quantify imaging-to-omics concordance and standardize spatial endpoints. Study registration: PROSPERO CRD420251113416. Funding: none.
Mots clés
MALDI mass spectrometry imaging (MALDI-MSI), amino acid PET (MET/FET/FDOPA), high-grade glioma, high-resolution magic angle spinning nuclear magnetic resonance (HR-MAS NMR) spectroscopy, positron emission tomography (PET), pseudoprogression, treatment-related change
Référence
Metabolites. 2025 12 24;16(1):
