PRMT5 inhibition disrupts splicing and stemness in glioblastoma

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作者
Patty Sachamitr
Jolene C. Ho
Felipe E. Ciamponi
Wail Ba-Alawi
Fiona J. Coutinho
Paul Guilhamon
Michelle M. Kushida
Florence M. G. Cavalli
Lilian Lee
Naghmeh Rastegar
Victoria Vu
María Sánchez-Osuna
Jasmin Coulombe-Huntington
Evgeny Kanshin
Heather Whetstone
Mathieu Durand
Philippe Thibault
Kirsten Hart
Maria Mangos
Joseph Veyhl
Wenjun Chen
Nhat Tran
Bang-Chi Duong
Ahmed M. Aman
Xinghui Che
Xiaoyang Lan
Owen Whitley
Olga Zaslaver
Dalia Barsyte-Lovejoy
Laura M. Richards
Ian Restall
Amy Caudy
Hannes L. Röst
Zahid Quyoom Bonday
Mark Bernstein
Sunit Das
Michael D. Cusimano
Julian Spears
Gary D. Bader
Trevor J. Pugh
Mike Tyers
Mathieu Lupien
Benjamin Haibe-Kains
H. Artee Luchman
Samuel Weiss
Katlin B. Massirer
Panagiotis Prinos
Cheryl H. Arrowsmith
Peter B. Dirks
机构
[1] The Hospital for Sick Children,Developmental and Stem Cell Biology Program and Arthur and Sonia Labatt Brain Tumor Research Centre
[2] University of Toronto,Structural Genomics Consortium
[3] University of Campinas (UNICAMP),Center for Molecular Biology and Genetic Engineering
[4] University of Campinas (UNICAMP),The Structural Genomics Consortium
[5] University Health Network,Princess Margaret Cancer Centre
[6] University of Toronto,Department of Medical Biophysics
[7] Université de Montréal,Institute for Research in Immunology and Cancer
[8] Université de Sherbrooke,RNomics Platform
[9] Ontario Institute for Cancer Research,The Donnelly Centre
[10] University of Toronto,Department of Molecular Genetics
[11] University of Toronto,Department of Pharmacology and Toxicology
[12] University of Toronto,Hotchkiss Brain Institute, Cumming School of Medicine
[13] University of Calgary,Department of Cell Biology and Anatomy
[14] University of Calgary,Lilly Research Laboratories
[15] Maple Flavored Solutions,Division of Neurosurgery, Department of Surgery
[16] LLC,Division of Neurosurgery, Toronto Western Hospital
[17] Eli Lilly and Company,Division of Neurosurgery, Department of Surgery
[18] University of Toronto,The Arthur and Sonia Labatt Brain Tumour Research Centre
[19] University Health Network,Department of Medical Imaging, St. Michael’s Hospital
[20] St. Michael’s Hospital,Department of Computer Science
[21] The Hospital for Sick Children,Clark H. Smith Brain Tumor Centre, Cumming School of Medicine
[22] University of Toronto,Department of Laboratory Medicine and Pathobiology
[23] University of Toronto,Division of Neurosurgery
[24] Vector Institute,undefined
[25] University of Calgary,undefined
[26] University of Toronto,undefined
[27] The Hospital for Sick Children,undefined
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摘要
Glioblastoma (GBM) is a deadly cancer in which cancer stem cells (CSCs) sustain tumor growth and contribute to therapeutic resistance. Protein arginine methyltransferase 5 (PRMT5) has recently emerged as a promising target in GBM. Using two orthogonal-acting inhibitors of PRMT5 (GSK591 or LLY-283), we show that pharmacological inhibition of PRMT5 suppresses the growth of a cohort of 46 patient-derived GBM stem cell cultures, with the proneural subtype showing greater sensitivity. We show that PRMT5 inhibition causes widespread disruption of splicing across the transcriptome, particularly affecting cell cycle gene products. We identify a GBM splicing signature that correlates with the degree of response to PRMT5 inhibition. Importantly, we demonstrate that LLY-283 is brain-penetrant and significantly prolongs the survival of mice with orthotopic patient-derived xenografts. Collectively, our findings provide a rationale for the clinical development of brain penetrant PRMT5 inhibitors as treatment for GBM.
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