Litcius/Paper detail

BMX controls 3βHSD1 and sex steroid biosynthesis in cancer

Xiuxiu Li, Michael Berk, Christopher M. Goins, Mohammad Alyamani, Yoon‐Mi Chung, Chenyao Wang, Monaben Patel, Nityam Rathi, Ziqi Zhu, Belinda Willard, Shaun R. Stauffer, Eric A. Klein, Nima Sharifi

2023Journal of Clinical Investigation28 citationsDOIOpen Access PDF

Abstract

Prostate cancer is highly dependent on androgens and the androgen receptor (AR). Hormonal therapies inhibit gonadal testosterone production, block extragonadal androgen biosynthesis, or directly antagonize AR. Resistance to medical castration occurs as castration-resistant prostate cancer (CRPC) and is driven by reactivation of the androgen-AR axis. 3β-hydroxysteroid dehydrogenase-1 (3βHSD1) serves as the rate-limiting step for potent androgen synthesis from extragonadal precursors, thereby stimulating CRPC. Genetic evidence in men demonstrates the role of 3βHSD1 in driving CRPC. In postmenopausal women, 3βHSD1 is required for synthesis of aromatase substrates and plays an essential role in breast cancer. Therefore, 3βHSD1 lies at a critical junction for the synthesis of androgens and estrogens, and this metabolic flux is regulated through germline-inherited mechanisms. We show that phosphorylation of tyrosine 344 (Y344) occurs and is required for 3βHSD1 cellular activity and generation of Δ4, 3-keto-substrates of 5α-reductase and aromatase, including in patient tissues. BMX directly interacts with 3βHSD1 and is necessary for enzyme phosphorylation and androgen biosynthesis. In vivo blockade of 3βHSD1 Y344 phosphorylation inhibits CRPC. These findings identify what we believe to be new hormonal therapy pharmacologic vulnerabilities for sex-steroid dependent cancers.

Topics & Concepts

AromataseAndrogenEndocrinologyProstate cancerAndrogen receptorInternal medicineTestosterone (patch)IntracrineCancer researchBiologyCancerMedicineHormoneReceptorBreast cancerParacrine signallingProstate Cancer Treatment and ResearchHormonal and reproductive studiesEstrogen and related hormone effects