Androgen actions via androgen receptor promote PTEN inactivation induced uterine cancer
- Jaesung (Peter) Choi,
- Reena Desai,
- Yu Zheng,
- Mu Yao1,
- Qihan Dong1,
- Geoff Watson2,
- David J Handelsman⇑ and
- Ulla Simanainen
- ANZAC Research Institute, University of Sydney, Sydney, New South Wales 2139, Australia
1Discipline of Endocrinology, Central Clinical School, Bosch Institute, Charles Perkins Centre, Royal Prince Alfred Hospital, University of Sydney, Sydney, New South Wales 2050, Australia
2Department of Anatomical Pathology, Royal Prince Alfred Hospital, Sydney, New South Wales 2050, Australia
- Correspondence should be addressed to D J Handelsman; Email: djh{at}anzac.edu.au
Abstract
Haploinsufficient inactivating phosphatase and tensin homolog (Pten) mutations cause Cowden syndrome, an autosomal dominant risk genotype for hormone dependent reproductive cancers. As androgen actions mediated via the androgen receptor (AR) supports uterine growth and may modify uterine cancer risk, we hypothesized that a functional AR may increase PTEN inactivation induced uterine cancer. To test the hypothesis, we compared the PTEN knockout (PTENKO) induced uterine pathology in heterozygous PTENKO and combined heterozygous PTEN and complete AR knockout (PTENARKO) female mice. PTENKO induced uterine pathology was significantly reduced by AR inactivation with severe macroscopic uterine pathology present in 21% of PTENARKO vs 46% of PTENKO at a median age of 45 weeks. This could be due to reduced stroma ERα expression in PTENARKO compared to PTENKO uterus, while AR inactivation did not modify PTEN or P-AKT levels. Unexpectedly, while progesterone (P4) is assumed protective in uterine cancers, serum P4 was significantly higher in PTENKO females compared to WT, ARKO, and PTENARKO females consistent with more corpora lutea in PTENKO ovaries. Serum testosterone and ovarian estradiol were similar between all females. Hence, our results demonstrated AR inactivation mediated protection against PTENKO induced uterine pathology and suggests a potential role for antiandrogens in uterine cancer prevention and treatment.
- Revision received 1 July 2015
- Accepted 6 July 2015
- © 2015 Society for Endocrinology