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Therapeutic targeting of the MYC signal by inhibition of histone chaperone FACT in neuroblastoma.


ABSTRACT: Amplification of the MYCN oncogene predicts treatment resistance in childhood neuroblastoma. We used a MYC target gene signature that predicts poor neuroblastoma prognosis to identify the histone chaperone FACT (facilitates chromatin transcription) as a crucial mediator of the MYC signal and a therapeutic target in the disease. FACT and MYCN expression created a forward feedback loop in neuroblastoma cells that was essential for maintaining mutual high expression. FACT inhibition by the small-molecule curaxin compound CBL0137 markedly reduced tumor initiation and progression in vivo. CBL0137 exhibited strong synergy with standard chemotherapy by blocking repair of DNA damage caused by genotoxic drugs, thus creating a synthetic lethal environment in MYCN-amplified neuroblastoma cells and suggesting a treatment strategy for MYCN-driven neuroblastoma.

SUBMITTER: Carter DR 

PROVIDER: S-EPMC6207083 | biostudies-literature | 2015 Nov

REPOSITORIES: biostudies-literature

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Therapeutic targeting of the MYC signal by inhibition of histone chaperone FACT in neuroblastoma.

Carter Daniel R DR   Murray Jayne J   Cheung Belamy B BB   Gamble Laura L   Koach Jessica J   Tsang Joanna J   Sutton Selina S   Kalla Heyam H   Syed Sarah S   Gifford Andrew J AJ   Issaeva Natalia N   Biktasova Asel A   Atmadibrata Bernard B   Sun Yuting Y   Sokolowski Nicolas N   Ling Dora D   Kim Patrick Y PY   Webber Hannah H   Clark Ashleigh A   Ruhle Michelle M   Liu Bing B   Oberthuer André A   Fischer Matthias M   Byrne Jennifer J   Saletta Federica F   Thwe Le Myo le M   Purmal Andrei A   Haderski Gary G   Burkhart Catherine C   Speleman Frank F   De Preter Katleen K   Beckers Anneleen A   Ziegler David S DS   Liu Tao T   Gurova Katerina V KV   Gudkov Andrei V AV   Norris Murray D MD   Haber Michelle M   Marshall Glenn M GM  

Science translational medicine 20151101 312


Amplification of the MYCN oncogene predicts treatment resistance in childhood neuroblastoma. We used a MYC target gene signature that predicts poor neuroblastoma prognosis to identify the histone chaperone FACT (facilitates chromatin transcription) as a crucial mediator of the MYC signal and a therapeutic target in the disease. FACT and MYCN expression created a forward feedback loop in neuroblastoma cells that was essential for maintaining mutual high expression. FACT inhibition by the small-mo  ...[more]

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