| Literature DB >> 28966034 |
Christian J Braun1, Monica Stanciu1, Paul L Boutz1, Jesse C Patterson1, David Calligaris2, Fumi Higuchi3, Rachit Neupane1, Silvia Fenoglio1, Daniel P Cahill3, Hiroaki Wakimoto3, Nathalie Y R Agar4, Michael B Yaffe5, Phillip A Sharp1, Michael T Hemann6, Jacqueline A Lees7.
Abstract
Glioblastoma (GBM) is a devastating malignancy with few therapeutic options. We identify PRMT5 in an in vivo GBM shRNA screen and show that PRMT5 knockdown or inhibition potently suppresses in vivo GBM tumors, including patient-derived xenografts. Pathway analysis implicates splicing in cellular PRMT5 dependency, and we identify a biomarker that predicts sensitivity to PRMT5 inhibition. We find that PRMT5 deficiency primarily disrupts the removal of detained introns (DIs). This impaired DI splicing affects proliferation genes, whose downregulation coincides with cell cycle defects, senescence and/or apoptosis. We further show that DI programs are evolutionarily conserved and operate during neurogenesis, suggesting that they represent a physiological regulatory mechanism. Collectively, these findings reveal a PRMT5-regulated DI-splicing program as an exploitable cancer vulnerability.Entities:
Keywords: CLNS1A; EPZ015666; GBM; PRMT5; RIOK1; biomarker; splicing addiction
Mesh:
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Year: 2017 PMID: 28966034 PMCID: PMC5929990 DOI: 10.1016/j.ccell.2017.08.018
Source DB: PubMed Journal: Cancer Cell ISSN: 1535-6108 Impact factor: 38.585