Journal
MOLECULAR NUTRITION & FOOD RESEARCH
Volume 60, Issue 11, Pages 2387-2395Publisher
WILEY
DOI: 10.1002/mnfr.201600048
Keywords
Black raspberry; Cell proliferation; Endometrial cancer; Estrogen receptor; Urolithin A
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Funding
- Clinical and Translational Scientific Institute (CTSI) of Southeast Wisconsin (NIH) [8UL 1TR000055]
- Women's Health Research Program
- Faculty Affairs Committee at the Medical College of Wisconsin
- Foundation of Women's Cancer
- NIH [R01 CA148818]
- American Cancer Society [RSG-13-138-01-CNE]
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Scope: Obese and overweight women are at high risk of developing endometrial cancer; indeed, many of endometrial cancer patients are obese. The increased number and size of adipocytes due to obesity elevate levels of circulating estrogens that stimulate cell proliferation in the endometrium. However, black raspberries are a promising approach to preventing endometrial cancer. Methods and results: We examined 17 black raspberry constituents and metabolites (10 mu M or 10 mu g/mL, 48 h) for their ability to prevent endometrial cancer cells from proliferating. Urolithin A (UA) was most able to suppress proliferation in a time- and dose-dependent manner (p < 0.05). It arrested the G2/M phase of the cell cycle by upregulating cyclin-B1, cyclin-E2, p21, phospho-cdc2, and CDC25B. UAalso acted as an estrogen agonist by modulating estrogen receptor-alpha (ER alpha) dependent gene expression in ER-positive endometrial cancer cells. UA enhanced the expression of ER beta, PGR, pS2, GREB1 while inhibiting the expression of ER alpha and GRIP1. Coincubating UA-treated cells with the estrogen antagonist ICI182,780 abolished UA's estrogenic effects. Knocking down ER alpha suppressed PGR, pS2, and GREB gene expression but increased GRIP1 expression. Thus, UA's actions appear to be mediated through ER alpha. Conclusion: This study suggests that UA modulates ER alpha-dependent gene expression, thereby inhibiting endometrial cancer proliferation.
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