ZNF397 deficiency triggers TET2-driven lineage plasticity and AR-targeted therapy resistance in prostate cancer Journal Article

   


Authors: Xu, Y.; Yang, Y.; Wang, Z.; Sjöström, M.; Jiang, Y.; Tang, Y.; Cheng, S.; Deng, S.; Wang, C.; Gonzalez, J.; Johnson, N. A.; Li, X.; Li, X.; Metang, L. A.; Mukherji, A.; Xu, Q.; Tirado, C. R.; Wainwright, G.; Yu, X.; Barnes, S.; Hofstad, M.; Chen, Y.; Zhu, H.; Hanker, A. B.; Raj, G. V.; Zhu, G.; He, H. H.; Wang, Z.; Arteaga, C. L.; Liang, H.; Feng, F. Y.; Wang, Y.; Wang, T.; Mu, P.
Article Title: ZNF397 deficiency triggers TET2-driven lineage plasticity and AR-targeted therapy resistance in prostate cancer
Abstract: Cancer cells exhibit phenotypical plasticity and epigenetic reprogramming that allows them to evade lineage-dependent targeted treatments by adopting lineage plasticity. The underlying mechanisms by which cancer cells exploit the epigenetic regulatory machinery to acquire lineage plasticity and therapy resistance remain poorly understood. We identified zinc finger protein 397 (ZNF397) as a bona fide coactivator of the androgen receptor (AR), essential for the transcriptional program governing AR-driven luminal lineage. ZNF397 deficiency facilitates the transition of cancer cell from an AR-driven luminal lineage to a ten-eleven translocation 2 (TET2)-driven lineage plastic state, ultimately promoting resistance to therapies inhibiting AR signaling. Intriguingly, our findings indicate that a TET2 inhibitor can eliminate the resistance to AR-targeted therapies in ZNF397-deficient tumors. These insights uncover a novel mechanism through which prostate cancer acquires lineage plasticity via epigenetic rewiring and offer promising implications for clinical interventions designed to overcome therapy resistance dictated by lineage plasticity. Significance: This study reveals a bifurcated role of ZNF397, and a TET2-driven epigenetic mechanism regulating tumor lineage plasticity and therapy response in prostate cancer, enhances the understanding of drug resistance, and unveils a new therapeutic strategy for overcoming androgen receptor-targeted therapy resistance. ©2024 The Authors; Published by the American Association for Cancer Research.
Keywords: dna binding protein; tet2 protein, human; genetics; dna-binding proteins; proto-oncogene proteins; mouse; animal; metabolism; animals; mice; drug resistance; pathology; drug resistance, neoplasm; cell line, tumor; cell lineage; prostatic neoplasms; epigenesis, genetic; prostate tumor; tumor cell line; androgen receptor; receptors, androgen; drug therapy; genetic epigenesis; ar protein, human; dioxygenase; humans; human; male; proto oncogene protein; dioxygenases
Journal Title: Cancer Discovery
Volume: 14
Issue: 8
ISSN: 2159-8274
Publisher: American Association for Cancer Research  
Date Published: 2024-08-01
Start Page: 1496
End Page: 1521
Language: English
DOI: 10.1158/2159-8290.Cd-23-0539
PUBMED: 38591846
PROVIDER: scopus
PMCID: PMC11285331
DOI/URL:

https://www.scopus.com/inward/record.uri?eid=2-s2.0-85200523904&doi=10.1158%2f2159-8290.CD-23-0539&partnerID=40&md5=74f8e90c60c36c9dd70094164101aefc
Notes: Article -- Source: Scopus
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  1. Yu Chen
    133 Chen
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