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Histone Lysine Methylation Dynamics Control EGFR DNA Copy-Number Amplification

Cancer Discov. 2020; 
Clarke TL, Tang R, Chakraborty D, Van Rechem C, Ji F, Mishra S, Ma A, Kaniskan Hü, Jin J, Lawrence MS, Sadreyev RI, Whetstine JR.
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Recombinant Proteins Membranes were washed three times in PBST the next day, incubated with goat anti-mouse IgG peroxidase conjugated secondary antibody (170-6516, Biorad) or goat anti-rabbit peroxidase conjugated secondary antibody (A00167, GenScript) at 1:2500 in 5% milk-PBST for at least 1hr at room temperature, washed 3 times with PBST and incubated in Lumi-Light western blotting substrate (12015200001, Roche) or SuperSignal West Pico PLUS Chemiluminiscent substrate (34577, ThermoScientific) for 2-4 min(s). Get A Quote

摘要

Acquired chromosomal DNA copy gains are a feature of many tumors; however, the mechanisms that underpin oncogene amplification are poorly understood. Recent studies have begun to uncover the importance of epigenetic states and histone lysine methyltransferases (KMT) and demethylases (KDM) in regulating transient site-specific DNA copy-number gains (TSSG). In this study, we reveal a critical interplay between a myriad of lysine methyltransferases and demethylases in modulating H3K4/9/27 methylation balance to control extrachromosomal amplification of the EGFR oncogene. This study further establishes that cellular signals (hypoxia and EGF) are able to directly promote EGFR amplification through modulation of the ... More

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