Apurinic/apyrimidinic endodeoxyribonuclease 1 (APE1) promotes stress granule formation via YBX1 phosphorylation in ovarian cancer

Author:

Mao Shuyu,Xie Chong,Liu Yufeng,Zhao Ye,Li Mengxia,Gao Han,Xiao Yue,Zou Yongkang,Zheng Zhiguo,Gao Ya,Xie Juan,Tian Bing,Wang Liangyan,Hua Yuejin,Xu HongORCID

Abstract

AbstractAPE1 is an essential gene involved in DNA damage repair, the redox regulation of transcriptional factors (TFs) and RNA processing. APE1 overexpression is common in cancers and correlates with poor patient survival. Stress granules (SGs) are phase-separated cytoplasmic assemblies that cells form in response to environmental stresses. Precise regulation of SGs is pivotal to cell survival, whereas their dysregulation is increasingly linked to diseases. Whether APE1 engages in modulating SG dynamics is worthy of investigation. In this study, we demonstrate that APE1 colocalizes with SGs and promotes their formation. Through phosphoproteome profiling, we discover that APE1 significantly alters the phosphorylation landscape of ovarian cancer cells, particularly the phosphoprofile of SG proteins. Notably, APE1 promotes the phosphorylation of Y-Box binding protein 1 (YBX1) at S174 and S176, leading to enhanced SG formation and cell survival. Moreover, expression of the phosphomutant YBX1 S174/176E mimicking hyperphosphorylation in APE1-knockdown cells recovered the impaired SG formation. These findings shed light on the functional importance of APE1 in SG regulation and highlight the importance of YBX1 phosphorylation in SG dynamics.

Funder

Zhejiang Provincial Outstanding Youth Science Foundation

National Key research and development program of china

national natural science foundation of China

major program of Shenzhen Bay Laboratory

Fundamental Research Funds for the Central Universities

Publisher

Springer Science and Business Media LLC

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