Lapatinib sensitivity in nasopharyngeal carcinoma is modulated by SIRT2-mediated FOXO3 deacetylation.

Sathid AimjongjunZimam MahmudYannasittha JiramongkolGlowi AlasiriShang YaoErnesto YagüeTavan JanvilisriEric Wing-Fai Lam

Published in: BMC cancer (2019)

Collectively, our results suggest the involvement of SIRT2-mediated FOXO3 deacetylation in Lapatinib response and sensitivity, and that SIRT2 can specifically antagonise the cytotoxicity of Lapatinib through mediating FOXO3 deacetylation in both sensitive and resistant NPC cells. The present findings also propose that SIRT2 can be an important biomarker for metastatic and Lapatinib resistant NPC and that targeting the SIRT2-FOXO3 axis may provide novel strategies for treating NPC and for overcoming chemoresistance.

Keyphrases

transcription factor
oxidative stress
ischemia reperfusion injury

positive breast cancer
signaling pathway
pi k akt

metastatic breast cancer
induced apoptosis
squamous cell carcinoma

small cell lung cancer
cell cycle arrest
endoplasmic reticulum stress