| Literature DB >> 34320350 |
Francesca De Bacco1, Francesca Orzan1, Jessica Erriquez2, Elena Casanova1, Ludovic Barault3, Raffaella Albano2, Antonio D'Ambrosio1, Viola Bigatto1, Gigliola Reato1, Monica Patanè4, Bianca Pollo4, Geoffrey Kuesters5, Carmine Dell'Aglio6, Laura Casorzo7, Serena Pellegatta4, Gaetano Finocchiaro8, Paolo M Comoglio9, Carla Boccaccio10.
Abstract
In glioblastoma (GBM), the most frequent and lethal brain tumor, therapies suppressing recurrently altered signaling pathways failed to extend survival. However, in patient subsets, specific genetic lesions can confer sensitivity to targeted agents. By exploiting an integrated model based on patient-derived stem-like cells, faithfully recapitulating the original GBMs in vitro and in vivo, here, we identify a human GBM subset (∼9% of all GBMs) characterized by ERBB3 overexpression and nuclear accumulation. ERBB3 overexpression is driven by inheritable promoter methylation or post-transcriptional silencing of the oncosuppressor miR-205 and sustains the malignant phenotype. Overexpressed ERBB3 behaves as a specific signaling platform for fibroblast growth factor receptor (FGFR), driving PI3K/AKT/mTOR pathway hyperactivation, and overall metabolic upregulation. As a result, ERBB3 inhibition by specific antibodies is lethal for GBM stem-like cells and xenotransplants. These findings highlight a subset of patients eligible for ERBB3-targeted therapy.Entities:
Keywords: ERBB3; FGF; HER3; MM121; cancer metabolism; cancer stem cell; glioblastoma; miR-205; seribantumab; target therapy
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Year: 2021 PMID: 34320350 DOI: 10.1016/j.celrep.2021.109455
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423