Histone H2A Lys130 acetylation epigenetically regulates androgen production in prostate cancer

Thanh Nguyen; Dhivya Sridaran; Surbhi Chouhan; Cody Weimholt; Audrey Wilson; Jingqin Luo; Tiandao Li; John Koomen; Bin Fang; Nagireddy Putluri; Arun Sreekumar; Felix Y. Feng; Kiran Mahajan; Nupam P. Mahajan

doi:10.1038/s41467-023-38887-7

Nature Communications (Jun 2023)

Histone H2A Lys130 acetylation epigenetically regulates androgen production in prostate cancer

Thanh Nguyen,
Dhivya Sridaran,
Surbhi Chouhan,
Cody Weimholt,
Audrey Wilson,
Jingqin Luo,
Tiandao Li,
John Koomen,
Bin Fang,
Nagireddy Putluri,
Arun Sreekumar,
Felix Y. Feng,
Kiran Mahajan,
Nupam P. Mahajan

Affiliations

Thanh Nguyen: Department of Surgery, Cancer Research Building, Washington University in St Louis
Dhivya Sridaran: Department of Surgery, Cancer Research Building, Washington University in St Louis
Surbhi Chouhan: Department of Surgery, Cancer Research Building, Washington University in St Louis
Cody Weimholt: Siteman Cancer Center, Cancer Research Building, Washington University in St Louis
Audrey Wilson: Department of Surgery, Cancer Research Building, Washington University in St Louis
Jingqin Luo: Division of Public Health Sciences, Cancer Research Building, Washington University in St Louis
Tiandao Li: Bioinformatics Research Core, Center of Regenerative Medicine, Department of Developmental Biology, Washington University at St. Louis
John Koomen: Molecular Oncology and Molecular Medicine, Moffitt Cancer Center
Bin Fang: Molecular Oncology and Molecular Medicine, Moffitt Cancer Center
Nagireddy Putluri: Dan L Duncan Comprehensive Cancer Center, Baylor College of Medicine
Arun Sreekumar: Dan L Duncan Comprehensive Cancer Center, Baylor College of Medicine
Felix Y. Feng: Helen Diller Family Comprehensive Cancer Center, University of California
Kiran Mahajan: Department of Surgery, Cancer Research Building, Washington University in St Louis
Nupam P. Mahajan: Department of Surgery, Cancer Research Building, Washington University in St Louis

DOI: https://doi.org/10.1038/s41467-023-38887-7
Journal volume & issue: Vol. 14, no. 1
pp. 1 – 19

Abstract

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Abstract The testicular androgen biosynthesis is well understood, however, how cancer cells gauge dwindling androgen to dexterously initiate its de novo synthesis remained elusive. We uncover dual-phosphorylated form of sterol regulatory element-binding protein 1 (SREBF1), pY673/951-SREBF1 that acts as an androgen sensor, and dissociates from androgen receptor (AR) in androgen deficient environment, followed by nuclear translocation. SREBF1 recruits KAT2A/GCN5 to deposit epigenetic marks, histone H2A Lys130-acetylation (H2A-K130ac) in SREBF1, reigniting de novo lipogenesis & steroidogenesis. Androgen prevents SREBF1 nuclear translocation, promoting T cell exhaustion. Nuclear SREBF1 and H2A-K130ac levels are significantly increased and directly correlated with late-stage prostate cancer, reversal of which sensitizes castration-resistant prostate cancer (CRPC) to androgen synthesis inhibitor, Abiraterone. Further, we identify a distinct CRPC lipid signature resembling lipid profile of prostate cancer in African American (AA) men. Overall, pY-SREBF1/H2A-K130ac signaling explains cancer sex bias and reveal synchronous inhibition of KAT2A and Tyr-kinases as an effective therapeutic strategy.

Published in Nature Communications

ISSN: 2041-1723 (Online)
Publisher: Nature Portfolio
Country of publisher: United Kingdom
LCC subjects: Science
Website: https://www.nature.com/ncomms/

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