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Targeting the p300/NONO axis sensitizes melanoma cells to BRAF inhibitors

Authors :
Feifei, Zhang
Xiaofeng, Tang
Song, Fan
Xia, Liu
Jun, Sun
Cheng, Ju
Yiping, Liang
Renfeng, Liu
Ruihao, Zhou
Bo, Yu
Changhua, Zhang
Zhiping, Zhang
Tiebang, Kang
Guofu, Huang
Xiao-Bin, Lv
Source :
Oncogene. 40(24)
Publication Year :
2020

Abstract

BRAF inhibitors (BRAFi) that target BRAF V600E kinase, a driver mutation found in 50% of melanomas, show a significant antitumor response, but the common emergence of acquired resistance remains a challenge. Abnormal expression of RAF isoforms CRAF and ARAF reactivates pERK1/2, which plays crucial roles in the acquisition of resistance of melanoma cells. However, the mechanisms of dysregulation of RAF isoforms in resistant melanoma cells remain unknown. Here, we identified NONO interacted with and stabilized both CRAF and ARAF in melanoma cells, and that NONO was acetylated at 198K by p300 acetyltransferase, which stabilized NONO via antagonizing its ubiquitination/degradation mediated by RNF8. The upregulation of both p300 and NONO promoted the rebound of pERK1/2 and the subsequent resistance of melanoma cells to BRAFi, and the activation of ERK1/2 in turn induced p300 to form a positive feedback loop in resistant melanoma cells. There was a positive correlation between p300 and NONO in resistant melanoma cells and clinical samples, and p300 inhibitor C646 overcame the resistance of resistant melanoma cells to BRAF inhibitors in vitro and in vivo. Our findings reveal that targeting the positive feedback loop of p300-NONO-CRAF/ARAF-pERK1/2 may be excellent strategies to overcome the resistance of BRAF inhibitors for melanoma patients.

Details

ISSN :
14765594
Volume :
40
Issue :
24
Database :
OpenAIRE
Journal :
Oncogene
Accession number :
edsair.pmid..........76d3bcbcb093ecaec7e7d13eea41faaf