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FoxO1 promotes ovarian cancer by increasing transcription and METTL14‐mediated m<sup>6</sup>A modification of SMC4

Liping Tan, Shuangan Wang, Shijia Huang, Yujuan Tie, Na Sai, Yichen Mao, Shuli Zhao, Yayi Hou, Huan Dou

2024Cancer Science15 citationsDOIOpen Access PDF

Abstract

Abstract The transcription factor forkhead box protein O1 (FoxO1) is closely related to the occurrence and development of ovarian cancer (OC), however its role and molecular mechanisms remain unclear. Herein, we found that FoxO1 was highly expressed in clinical samples of OC patients and was significantly correlated with poor prognosis. FoxO1 knockdown inhibited the proliferation of OC cells in vitro and in vivo. ChIP‐seq combined with GEPIA2 and Kaplan–Meier database analysis showed that structural maintenance of chromosome 4 (SMC4) is a downstream target of FoxO1, and FoxO1 promotes SMC4 transcription by binding to its −1400/−1390 bp promoter. The high expression of SMC4 significantly blocked the tumor inhibition effect of FoxO1 knockdown. Furtherly, FoxO1 increased SMC4 mRNA abundance by transcriptionally activating methyltransferase‐like 14 (METTL14) and increasing SMC4 m 6 A methylation on its coding sequence region. The Cancer Genome Atlas dataset analysis confirmed a significant positive correlation between FoxO1, SMC4, and METTL14 expression in OC. In summary, this study revealed the molecular mechanisms of FoxO1 regulating SMC4 and established a clinical link between the expression of FoxO1/METTL14/SMC4 in the occurrence of OC, thus providing a potential diagnostic target and therapeutic strategy.

Topics & Concepts

FOXO1Gene knockdownTranscription factorCancer researchBiologyIn vivoOvarian cancerMolecular biologyChemistryCancerGeneGeneticsRNA modifications and cancerCancer-related molecular mechanisms researchRNA Research and Splicing
FoxO1 promotes ovarian cancer by increasing transcription and METTL14‐mediated m<sup>6</sup>A modification of SMC4 | Litcius