A feedback loop between the androgen receptor and 6-phosphogluoconate dehydrogenase (6PGD) drives prostate cancer growth-Reference-Cited by-同舟云学术

A feedback loop between the androgen receptor and 6-phosphogluoconate dehydrogenase (6PGD) drives prostate cancer growth

Published:2021-08-12 Issue: Volume:10 Page:
ISSN:2050-084X
Container-title:eLife
language:en
Short-container-title:

Author:

Gillis Joanna L¹²,Hinneh Josephine A¹²³,Ryan Natalie K¹²,Irani Swati¹²,Moldovan Max²,Quek Lake-Ee⁴,Shrestha Raj K¹⁵⁶⁷,Hanson Adrienne R⁵,Xie Jianling⁵,Hoy Andrew J⁸^ORCID,Holst Jeff⁹^ORCID,Centenera Margaret M¹²⁷,Mills Ian G¹⁰¹¹,Lynn David J²⁵,Selth Luke A¹⁵⁶⁷^ORCID,Butler Lisa M¹²⁷^ORCID

Affiliation:

1. Adelaide Medical School, University of Adelaide

2. South Australian Health and Medical Research Institute

3. Department of Urology, Nagoya University Graduate School of Medicine

4. School of Mathematics and Statistics, Charles Perkins Centre, Faculty of Science, The University of Sydney

5. Flinders Health and Medical Research Institute, Flinders University, College of Medicine and Public Health

6. Dame Roma Mitchell Cancer Research Laboratories, University of Adelaide

7. Freemasons Centre for Male Health and Wellbeing, University of Adelaide

8. School of Medical Sciences, Charles Perkins Centre, Faculty of Medicine and Health, The University of Sydney

9. School of Medical Sciences and Prince of Wales Clinical School, University of New South Wales

10. Centre for Cancer Research and Cell Biology, Queen's University Belfast

11. Nuffield Department of Surgical Sciences, University of Oxford

Abstract

Alterations to the androgen receptor (AR) signalling axis and cellular metabolism are hallmarks of prostate cancer. This study provides insight into both hallmarks by uncovering a novel link between AR and the pentose phosphate pathway (PPP). Specifically, we identify 6-phosphogluoconate dehydrogenase (6PGD) as an androgen-regulated gene that is upregulated in prostate cancer. AR increased the expression of 6PGD indirectly via activation of sterol regulatory element binding protein 1 (SREBP1). Accordingly, loss of 6PGD, AR or SREBP1 resulted in suppression of PPP activity as revealed by 1,2-13C2 glucose metabolic flux analysis. Knockdown of 6PGD also impaired growth and elicited death of prostate cancer cells, at least in part due to increased oxidative stress. We investigated the therapeutic potential of targeting 6PGD using two specific inhibitors, physcion and S3, and observed substantial anti-cancer activity in multiple models of prostate cancer, including aggressive, therapy-resistant models of castration-resistant disease as well as prospectively collected patient-derived tumour explants. Targeting of 6PGD was associated with two important tumour-suppressive mechanisms: first, increased activity of the AMP-activated protein kinase (AMPK), which repressed anabolic growth-promoting pathways regulated by acetyl-CoA carboxylase 1 (ACC1) and mammalian target of rapamycin complex 1 (mTORC1); and second, enhanced AR ubiquitylation, associated with a reduction in AR protein levels and activity. Supporting the biological relevance of positive feedback between AR and 6PGD, pharmacological co-targeting of both factors was more effective in suppressing the growth of prostate cancer cells than single-agent therapies. Collectively, this work provides new insight into the dysregulated metabolism of prostate cancer and provides impetus for further investigation of co-targeting AR and the PPP as a novel therapeutic strategy.

Funder

Cancer Australia

Movember Foundation

Prostate Cancer Foundation of Australia

Cancer Council South Australia

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

Link

https://cdn.elifesciences.org/articles/62592/elife-62592-v2.pdf

Reference59 articles.