Effects of Benzophenone-3 and Propylparaben on Estrogen Receptor–Dependent R-Loops and DNA Damage in Breast Epithelial Cells and Mice

交易激励 DNA损伤 雌激素受体 雌激素受体α 免疫染色 生物 雌激素受体 分子生物学 雌激素 辅活化剂 遗传毒性 内分泌学 化学 基因表达 癌症研究 内科学 DNA 基因 乳腺癌 免疫学 毒性 癌症 免疫组织化学 转录因子 医学 生物化学 遗传学
作者
Prabin D. Majhi,Aman Sharma,Amy L. Roberts,Elizabeth Daniele,A Majewski,Lynn M. Chuong,Amye L. Black,Laura N. Vandenberg,Sallie S. Schneider,Karen A. Dunphy,D. Joseph Jerry
出处
期刊:Environmental Health Perspectives [National Institute of Environmental Health Sciences]
卷期号:128 (1) 被引量:52
标识
DOI:10.1289/ehp5221
摘要

Background: Endocrine-disrupting chemicals have been shown to have broad effects on development, but their mutagenic actions that can lead to cancer have been less clearly demonstrated. Physiological levels of estrogen have been shown to stimulate DNA damage in breast epithelial cells through mechanisms mediated by estrogen-receptor alpha (ERα). Benzophenone-3 (BP-3) and propylparaben (PP) are xenoestrogens found in the urine of >96% of U.S. population. Objectives: We investigated the effect of BP-3 and PP on estrogen receptor–dependent transactivation and DNA damage at concentrations relevant to exposures in humans. Methods: In human breast epithelial cells, DNA damage following treatment with 17β-estradiol (E2), BP-3, and PP was determined by immunostaining with antibodies against γ-H2AX and 53BP1. Estrogenic responses were determined using luciferase reporter assays and gene expression. Formation of R-loops was determined with DNA: RNA hybrid–specific S9.6 antibody. Short-term exposure to the chemicals was also studied in ovariectomized mice. Immunostaining of mouse mammary epithelium was performed to quantify R-loops and DNA damage in vivo. Results: Concentrations of 1μM and 5μM BP-3 or PP increased DNA damage similar to that of E2 treatment in a ERα-dependent manner. However, BP-3 and PP had limited transactivation of target genes at 1μM and 5μM concentrations. BP-3 and PP exposure caused R-loop formation in a normal human breast epithelial cell line when ERα was introduced. R-loops and DNA damage were also detected in mammary epithelial cells of mice treated with BP-3 and PP. Conclusions: Acute exposure to xenoestrogens (PP and BP-3) in mice induce DNA damage mediated by formation of ERα-dependent R-loops at concentrations 10-fold lower than those required for transactivation. Exposure to these xenoestrogens may cause deleterious estrogenic responses, such as DNA damage, in susceptible individuals. https://doi.org/10.1289/EHP5221
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