The long noncoding RNA lncNB1 promotes tumorigenesis by interacting with ribosomal protein RPL35

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作者
Pei Y. Liu
Andrew E. Tee
Giorgio Milazzo
Katherine M. Hannan
Jesper Maag
Sujanna Mondal
Bernard Atmadibrata
Nenad Bartonicek
Hui Peng
Nicholas Ho
Chelsea Mayoh
Roberto Ciaccio
Yuting Sun
Michelle J. Henderson
Jixuan Gao
Celine Everaert
Amy J. Hulme
Matthew Wong
Qing Lan
Belamy B. Cheung
Leming Shi
Jenny Y. Wang
Thorsten Simon
Matthias Fischer
Xu D. Zhang
Glenn M. Marshall
Murray D. Norris
Michelle Haber
Jo Vandesompele
Jinyan Li
Pieter Mestdagh
Ross D. Hannan
Marcel E. Dinger
Giovanni Perini
Tao Liu
机构
[1] Children’s Cancer Institute Australia for Medical Research,Department of Pharmacy and Biotechnology
[2] University of Bologna,Australian Cancer Research Foundation Department of Cancer Biology and Therapeutics, The John Curtin School of Medical Research
[3] The Australian National University,Department of Biochemistry and Molecular Biology
[4] University of Melbourne,Center for Epigenetics Research
[5] Garvan Institute of Medical Research,Advanced Analytics Institute
[6] Sydney,Center for Medical Genetics Ghent
[7] Memorial Sloan Kettering Cancer Center,Department of Neurosurgery
[8] University of Technology Sydney,State Key Laboratory of Genetic Engineering, School of Life Sciences and Human Phenome Institute
[9] Ghent University,Department of Pediatric Oncology and Hematology
[10] the Second Affiliated Hospital of Soochow University,Department of Experimental Pediatric Oncology, University Hospital
[11] Fudan University,School of Medicine and Public Health, Priority Research Centre for Cancer Research
[12] University Hospital,Kids Cancer Centre
[13] University of Cologne,Sir Peter MacCallum Department of Oncology
[14] University of Cologne,Department of Biochemistry and Molecular Biology
[15] University of Newcastle,School of Biomedical Sciences
[16] Sydney Children’s Hospital,School of Biotechnology and Biomolecular Sciences
[17] University of Melbourne,undefined
[18] Monash University,undefined
[19] University of Queensland,undefined
[20] University of New South Wales,undefined
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摘要
The majority of patients with neuroblastoma due to MYCN oncogene amplification and consequent N-Myc oncoprotein over-expression die of the disease. Here our analyses of RNA sequencing data identify the long noncoding RNA lncNB1 as one of the transcripts most over-expressed in MYCN-amplified, compared with MYCN-non-amplified, human neuroblastoma cells and also the most over-expressed in neuroblastoma compared with all other cancers. lncNB1 binds to the ribosomal protein RPL35 to enhance E2F1 protein synthesis, leading to DEPDC1B gene transcription. The GTPase-activating protein DEPDC1B induces ERK protein phosphorylation and N-Myc protein stabilization. Importantly, lncNB1 knockdown abolishes neuroblastoma cell clonogenic capacity in vitro and leads to neuroblastoma tumor regression in mice, while high levels of lncNB1 and RPL35 in human neuroblastoma tissues predict poor patient prognosis. This study therefore identifies lncNB1 and its binding protein RPL35 as key factors for promoting E2F1 protein synthesis, N-Myc protein stability and N-Myc-driven oncogenesis, and as therapeutic targets.
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