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DOI: 10.1158/2159-8290.cd-12-0418
¤ OpenAccess: Bronze
This work has “Bronze” OA status. This means it is free to read on the publisher landing page, but without any identifiable license.

Targeting MYCN in Neuroblastoma by BET Bromodomain Inhibition

Alexandre Puissant,Stacey M. Frumm,Gabriela Alexe,Christopher F. Bassil,Jun Qi,Yvan H. Chanthery,Erin A. Nekritz,Rhamy Zeid,W. Clay Gustafson,Patricia Greninger,Matthew J. Garnett,Ultan McDermott,Cyril H. Benes,Andrew L. Kung,William A. Weiss,James E. Bradner,Kimberly Stegmaier

Bromodomain
Neuroblastoma
BRD4
2013
Bromodomain inhibition comprises a promising therapeutic strategy in cancer, particularly for hematologic malignancies. To date, however, genomic biomarkers to direct clinical translation have been lacking. We conducted a cell-based screen of genetically defined cancer cell lines using a prototypical inhibitor of BET bromodomains. Integration of genetic features with chemosensitivity data revealed a robust correlation between MYCN amplification and sensitivity to bromodomain inhibition. We characterized the mechanistic and translational significance of this finding in neuroblastoma, a childhood cancer with frequent amplification of MYCN. Genome-wide expression analysis showed downregulation of the MYCN transcriptional program accompanied by suppression of MYCN transcription. Functionally, bromodomain-mediated inhibition of MYCN impaired growth and induced apoptosis in neuroblastoma. BRD4 knockdown phenocopied these effects, establishing BET bromodomains as transcriptional regulators of MYCN. BET inhibition conferred a significant survival advantage in 3 in vivo neuroblastoma models, providing a compelling rationale for developing BET bromodomain inhibitors in patients with neuroblastoma.
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    Targeting MYCN in Neuroblastoma by BET Bromodomain Inhibition” is a paper by Alexandre Puissant Stacey M. Frumm Gabriela Alexe Christopher F. Bassil Jun Qi Yvan H. Chanthery Erin A. Nekritz Rhamy Zeid W. Clay Gustafson Patricia Greninger Matthew J. Garnett Ultan McDermott Cyril H. Benes Andrew L. Kung William A. Weiss James E. Bradner Kimberly Stegmaier published in 2013. It has an Open Access status of “bronze”. You can read and download a PDF Full Text of this paper here.