Loss of ESRP2 Activates TAK1‐MAPK Signaling through the Fetal RNA‐Splicing Program to Promote Hepatocellular Carcinoma Progression

Qian Yan; Xiaona Fang; Xiaoxia Liu; Sai Guo; Siqi Chen; Min Luo; Ping Lan; Xin‐Yuan Guan

doi:10.1002/advs.202305653

Advanced Science (Jan 2024)

Loss of ESRP2 Activates TAK1‐MAPK Signaling through the Fetal RNA‐Splicing Program to Promote Hepatocellular Carcinoma Progression

Qian Yan,
Xiaona Fang,
Xiaoxia Liu,
Sai Guo,
Siqi Chen,
Min Luo,
Ping Lan,
Xin‐Yuan Guan

Affiliations

Qian Yan: Guangdong Provincial Key Laboratory of Colorectal and Pelvic Floor Diseases Guangdong Institute of Gastroenterology The Sixth Affiliated Hospital Sun Yat‐sen University Guangzhou 510655 China
Xiaona Fang: Sun Yat‐sen University Cancer Center; State Key Laboratory of Oncology in South China; Collaborative Innovation Center for Cancer Medicine Guangzhou 510060 China
Xiaoxia Liu: Guangdong Provincial Key Laboratory of Colorectal and Pelvic Floor Diseases Guangdong Institute of Gastroenterology The Sixth Affiliated Hospital Sun Yat‐sen University Guangzhou 510655 China
Sai Guo: Shenzhen Traditional Chinese Medicine Hospital Shenzhen China
Siqi Chen: Guangdong Provincial Key Laboratory of Colorectal and Pelvic Floor Diseases Guangdong Institute of Gastroenterology The Sixth Affiliated Hospital Sun Yat‐sen University Guangzhou 510655 China
Min Luo: Department of Clinical Oncology The University of Hong Kong‐Shenzhen Hospital Shenzhen China
Ping Lan: Guangdong Provincial Key Laboratory of Colorectal and Pelvic Floor Diseases Guangdong Institute of Gastroenterology The Sixth Affiliated Hospital Sun Yat‐sen University Guangzhou 510655 China
Xin‐Yuan Guan: Department of Clinical Oncology The University of Hong Kong‐Shenzhen Hospital Shenzhen China

DOI: https://doi.org/10.1002/advs.202305653
Journal volume & issue: Vol. 11, no. 1
pp. n/a – n/a

Abstract

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Abstract Tumors usually display fetal‐like characteristics, and many oncofetal proteins have been identified. However, fetal‐like reprogramming of RNA splicing in hepatocellular carcinoma (HCC) is poorly understood. Here, it is demonstrated that the expression of epithelial splicing regulatory protein 2 (ESRP2), an RNA splicing factor, is suppressed in fetal hepatocytes and HCC, in parallel with tumor progression. By combining RNA‐Seq with splicing analysis, it is identified that ESRP2 controls the fetal‐to‐adult switch of multiple splice isoforms in HCC. Functionally, ESRP2 suppressed cell proliferation and migration by specifically switching the alternative splicing (AS) of the TAK1 gene and restraining the expression of the fetal and oncogenic isoform, TAK1_ΔE12. Notably, aberrant TAK1 splicing led to the activation of p38MAPK signaling and predicted poor prognosis in HCC patients. Further investigation revealed that TAK1_ΔE12 protein interacted closely with TAB3 and formed liquid condensation in HCC cells, resulting in p38MAPK activation, enhanced cell migration, and accelerated tumorigenesis. Loss of ESRP2 sensitized HCC cells to TAK1 kinase inhibitor (TAK1i), promoting pyroptotic cell death and CD8+ T cell infiltration. Combining TAK1i with immune checkpoint therapy achieved potent tumor regression in mice. Overall, the findings reveal a previously unexplored onco‐fetal reprogramming of RNA splicing and provide novel therapeutic avenues for HCC.

Published in Advanced Science

ISSN: 2198-3844 (Online)
Publisher: Wiley
Country of publisher: Germany
LCC subjects: Science
Website: https://onlinelibrary.wiley.com/journal/21983844

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