| Literature DB >> 22157079 |
Jessica D Kessler1, Kristopher T Kahle, Tingting Sun, Kristen L Meerbrey, Michael R Schlabach, Earlene M Schmitt, Samuel O Skinner, Qikai Xu, Mamie Z Li, Zachary C Hartman, Mitchell Rao, Peng Yu, Rocio Dominguez-Vidana, Anthony C Liang, Nicole L Solimini, Ronald J Bernardi, Bing Yu, Tiffany Hsu, Ido Golding, Ji Luo, C Kent Osborne, Chad J Creighton, Susan G Hilsenbeck, Rachel Schiff, Chad A Shaw, Stephen J Elledge, Thomas F Westbrook.
Abstract
Myc is an oncogenic transcription factor frequently dysregulated in human cancer. To identify pathways supporting the Myc oncogenic program, we used a genome-wide RNA interference screen to search for Myc-synthetic lethal genes and uncovered a role for the SUMO-activating enzyme (SAE1/2). Loss of SAE1/2 enzymatic activity drives synthetic lethality with Myc. Inactivation of SAE2 leads to mitotic catastrophe and cell death upon Myc hyperactivation. Mechanistically, SAE2 inhibition switches a transcriptional subprogram of Myc from activated to repressed. A subset of these SUMOylation-dependent Myc switchers (SMS genes) is required for mitotic spindle function and to support the Myc oncogenic program. SAE2 is required for growth of Myc-dependent tumors in mice, and gene expression analyses of Myc-high human breast cancers suggest that low SAE1 and SAE2 abundance in the tumors correlates with longer metastasis-free survival of the patients. Thus, inhibition of SUMOylation may merit investigation as a possible therapy for Myc-driven human cancers.Entities:
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Year: 2011 PMID: 22157079 PMCID: PMC4059214 DOI: 10.1126/science.1212728
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728