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苯并(a)芘降低了底鳉大脑和卵巢中芳香化酶mRNA的表达。

Benzo(a)pyrene decreases brain and ovarian aromatase mRNA expression in Fundulus heteroclitus.

作者信息

Dong Wu, Wang Lu, Thornton Cammi, Scheffler Brian E, Willett Kristine L

机构信息

Department of Pharmacology, School of Pharmacy, University of Mississippi, MS 38677, United States.

出版信息

Aquat Toxicol. 2008 Jul 30;88(4):289-300. doi: 10.1016/j.aquatox.2008.05.006. Epub 2008 May 15.

Abstract

The higher molecular weight polycyclic aromatic hydrocarbons (PAHs) such as benzo(a)pyrene (BaP) are typically associated with genotoxicity, however, newer evidence suggests that these compounds may also act as endocrine system disruptors. We hypothesized that altered expression of the P450 enzyme aromatase genes could be a target for reproductive or developmental dysfunction caused by BaP exposure. Aromatase is at least partially responsible for estrogen homeostasis by converting androgens into estrogens. In fish, there are two isoforms of aromatase, a predominantly ovarian form, CYP19A1, and a brain form, CYP19A2. CYP19 mRNA expression was measured following BaP exposure (0, 10, 100 microg/L waterborne for 10 or 15 days) in Fundulus adults, juveniles and embryos by in situ hybridization. The CYP19A1 expression was significantly decreased after BaP exposure in the 3-month-old Fundulus immature oocytes, but BaP did not affect CYP19A1 expression at any stage in adult oocytes. In embryo brains, BaP significantly decreased CYP19A2 compared to controls by 3.6-fold at 14 days post-fertilization. In adults, CYP19A2 expression was decreased significantly in the pituitary and hypothalamus (81% and 85% of controls, respectively). Promoter regions of Fundulus CYP19s were cloned, and putative response elements in the CYP19A1 and CYP19A2 promoters such as CRE, AhR and ERE may be involved in BaP-mediated changes in CYP19 expression. In order to compare the mechanism of BaP-mediated inhibition with that of a known aromatase inhibitor, fish were also exposed to fadrozole (20 and 100 microg/L). Fadrozole did not significantly decrease the mRNA expression in embryos or adult Fundulus. However, aromatase enzyme activity was significantly decreased in adult ovary and brain tissues. These studies provide a greater molecular understanding of the mechanisms of action of BaP and its potential to impact reproduction or development.

摘要

较高分子量的多环芳烃(PAHs),如苯并(a)芘(BaP),通常与遗传毒性有关,然而,新的证据表明这些化合物也可能作为内分泌系统干扰物。我们假设,P450酶芳香化酶基因表达的改变可能是BaP暴露导致生殖或发育功能障碍的一个靶点。芳香化酶通过将雄激素转化为雌激素,至少部分负责雌激素的稳态。在鱼类中,芳香化酶有两种同工型,一种主要是卵巢型,CYP19A1,另一种是脑型,CYP19A2。通过原位杂交在Fundulus成鱼、幼鱼和胚胎中测量了BaP暴露(0、10、100μg/L水体,暴露10或15天)后的CYP19 mRNA表达。在3个月大的Fundulus未成熟卵母细胞中,BaP暴露后CYP19A1表达显著降低,但BaP在成年卵母细胞的任何阶段都不影响CYP19A1表达。在胚胎大脑中,与对照组相比,受精后14天BaP使CYP19A2显著降低了3.6倍。在成鱼中,垂体和下丘脑的CYP19A2表达显著降低(分别为对照组的81%和85%)。克隆了Fundulus CYP19s的启动子区域,CYP19A1和CYP19A2启动子中的假定反应元件,如CRE、AhR和ERE,可能参与了BaP介导的CYP19表达变化。为了比较BaP介导的抑制机制与已知芳香化酶抑制剂的抑制机制,鱼类也暴露于法倔唑(20和100μg/L)。法倔唑并未显著降低胚胎或成年Fundulus中的mRNA表达。然而,成年卵巢和脑组织中的芳香化酶活性显著降低。这些研究为BaP的作用机制及其对生殖或发育的潜在影响提供了更深入的分子理解。

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