Publication | Open Access
Anti-tumor effect of estrogen-related receptor alpha knockdown on uterine endometrial cancer
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Citations
37
References
2016
Year
Estrogen ReceptorGynecologyCell DeathCancer BiologyMammary Gland DevelopmentTumor BiologyEstrogen-related ReceptorCancer Cell BiologyUterine Endometrial CancerCancer ResearchHormonal ReceptorEndocrinologyPharmacologyCell BiologyOvarian HormoneEndocrine-related CancerAnti-tumor EffectEndometrial Cancer ProgressionUterine ReceptivityEndometrial CancerMedicineCancer Growth
Estrogen-related receptor (ERR)α presents structural similarities with estrogen receptor (ER)α. However, it is an orphan receptor not binding to naturally occurring estrogens. This study was designed to investigate the role of ERRα in endometrial cancer progression. Immunohistochemistry analysis on 50 specimens from patients with endometrial cancer showed that ERRα was expressed in all examined tissues and the elevated expression levels of ERRα were associated with advanced clinical stages and serous histological type (p < 0.01 for each). ERRα knockdown with siRNA suppressed angiogenesis via VEGF and cell proliferation in vitro (p < 0.01). Cell cycle and apoptosis assays using flow cytometry and western blot revealed that ERRα knockdown induced cell cycle arrest during the mitotic phase followed by apoptosis initiated by caspase-3. Additionally, ERRα knockdown sensitized cells to paclitaxel. A significant reduction of tumor growth and angiogenesis was also observed in ERRα knockdown xenografts (p < 0.01). These findings indicate that ERRα may serve as a novel molecular target for the treatment of endometrial cancer.
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