par Cantero, Diana;Rodrıguez De Lope, Angel;Moreno De La Presa, Raquel;Sepulveda, Juan Manuel;Borras, José Matesanz;Castresana, J.S.;D'Haene, Nicky 
;Garcıa, Juán Fernando;Salmon, Isabelle ;Mollejo, Manuela;Rey, Juan Antonio;Hernandez-Laın, Aurelio;Melendez, Barbara
Référence Journal of neuropathology and experimental neurology, 77, 8, page (710-716)
Publication Publié, 2018
;Garcıa, Juán Fernando;Salmon, Isabelle ;Mollejo, Manuela;Rey, Juan Antonio;Hernandez-Laın, Aurelio;Melendez, BarbaraRéférence Journal of neuropathology and experimental neurology, 77, 8, page (710-716)
Publication Publié, 2018
Article révisé par les pairs
| Résumé : | Glioblastoma (GBM) is the most common malignant adult primary brain tumor. Despite its high lethality, a small proportion of patients have a relatively long overall survival (OS). Here we report a study of a series of 74 GBM samples from 29 long-term survivors ([LTS] OS 36 months) and 45 non-LTS. Using next-generation sequencing, we analyzed genetic alterations in the genes most frequently altered in gliomas. Approximately 20% of LTS had a mutation in the IDH1 or IDH2 (IDH) genes, denoting the relevance of this molecular prognostic factor. A new molecular group of GBMs harbored alterations in ATRX or DAXX genes in the absence of driver IDH or H3F3A mutations. These patients tended to have a slightly better prognosis, to be younger at diagnosis, and to present frontal or temporal tumors, and, morphologically, to present giant tumor cells. A significant fraction of LTS GBM patients had tumors with 1 or more alterations in the relevant GBM signaling pathways (RTK/PI3K, TP53 and RB1). In these patients, the PDGFRA alteration is suggested to be a favorable molecular factor. Our findings here are relevant for developing future targeted therapies and for identifying molecular prognostic factors in GBM patients. |
