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ERβ modulates genistein’s cisplatin-enhancing activities in breast cancer MDA-MB-231 cells via P53-independent pathway

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As one of the typical food-derived phytoestrogens, genistein (GEN) could bind to estrogen receptor (ER) and was reported to be closely related to breast cancer. Our former research showed that… Click to show full abstract

As one of the typical food-derived phytoestrogens, genistein (GEN) could bind to estrogen receptor (ER) and was reported to be closely related to breast cancer. Our former research showed that GEN interfered with the anti-tumor effects of cisplatin (CIS) in breast cancer MCF-7 (ERα+/ERβ−) cells. However, it is not clear whether ER expression pattern affects GEN’s modulation on CIS’s activity. In the present study, breast cancer ERβ knockdown (ERβKD) MDA-MB-231 (ERα−/ERβ+) cell model was established via ERβ RNAi lentivirus infection. The role of ERβ expression in GEN’s bioeffects on cells’ response to CIS was investigated and was further double-checked by pathway-specific inhibitor PHTPP. Consistent results were harvested through cell viability analysis, cell cycle distribution flow cytometry, TUNEL staining, and expression detection of key biomarkers, Bax, Bcl-2, P21, P53, and cleaved caspase-3. Compared with the control group, PHTPP-treated or ERβKD cells exhibited higher sensitivity to both GEN and CIS treatment. GEN and CIS showed synergistic effects only in ERβ-deficient cells. This effect mainly resulted in G2 phase arresting and apoptosis induction with the upregulation of P21 and Bax/Bcl-2 protein level. Besides, P53 expression was strikingly suppressed in ERβ-deficient cells. This indicated ERβ pathway deficiency might enhance GEN–CIS bioactivity via the downregulation of P53. In summary, our data imply that daily intake of GEN-rich diet could collaborate with CIS anti-tumor treatment in ERα−/ERβ− breast cancer cases. ERβ pathway might be one of the potential targets which elicit GEN’s positive effects in ERα− breast cancer patients.

Keywords: cis; mda 231; gen; breast cancer; p53

Journal Title: Molecular and Cellular Biochemistry
Year Published: 2019

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