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ER stress activates TAp73α to promote colon cancer cell apoptosis via the PERK-ATF4 pathway

Shengnan Sun, Yong Yi, Zhi‐Xiong Jim Xiao, Hu Chen

2023Journal of Cancer21 citationsDOIOpen Access PDF

Abstract

. Knockdown of TAp73α partially restores ER stress-induced apoptosis, indicating that ER stress stimulates apoptosis in a manner dependent on TAp73α, but not p53. Furthermore, we found that ER stress activates TAp73α mRNA and protein expression through PERK signalling, a branch of the unfolded protein response (UPR). Moreover, PERK promotes TAp73α expression by upregulating the expression of the transcription factor ATF4. ATF4 directly activates the transcription of TAp73α. Consistent with this finding, ATF4 knockdown inhibited PERK- or ER stress-induced TAp73α expression. Our findings reveal that ER stress activates TAp73α to promote colon cancer cell apoptosis via the PERK-ATF4 signalling. Therefore, prolonged ER stress or upregulation of TAp73α might be a therapeutic strategy for colon cancer.

Topics & Concepts

Unfolded protein responseGene knockdownATF4ApoptosisCancer researchDownregulation and upregulationEndoplasmic reticulumProgrammed cell deathTranscription factorCell biologyBiologyGeneBiochemistryEndoplasmic Reticulum Stress and DiseaseRNA regulation and diseaseHeat shock proteins research
ER stress activates TAp73α to promote colon cancer cell apoptosis via the PERK-ATF4 pathway | Litcius