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首页> 外文期刊>Archives of Toxicology >Progesterone, as well as 17 beta-estradiol, is important for regulating AHR battery homoeostasis in the rat uterus
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Progesterone, as well as 17 beta-estradiol, is important for regulating AHR battery homoeostasis in the rat uterus

机译:孕酮以及17β-雌二醇对于调节大鼠子宫AHR电池的稳态具有重要作用

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Several studies indicate that the aryl hydrocarbon receptor (AHR), which plays an important role in mediating the toxicity of many industrial chemicals, plays an important role in the physiology of female reproductive tract organs. This makes it likely that the AHR and additional components of the AHR signalling pathway are under the control of female sex steroids. In a previous study, we could already demonstrate the regulation of many members of the AHR battery by 17 beta-estradiol (E2) in the uterus of rats. In this study, we addressed the potential role of progesterone (P4) in this context. In a comparative approach using ovariectomized rats which were treated for 3 days with either vehicle control, E2, progesterone (P4) or the combination of both hormones in addition to sham-operated animals, we could demonstrate that in addition to E2, P4 is also an important factor in regulating AHR signalling in the rat uterus. P4 has effects similar to E2 on uterine Ahr, Arnt and Arnt2 mRNA levels, resulting in a downregulation of these genes, while the E2-mediated downregulation of key AHR response genes Cyp1a1, Gsta2 and Ugt1 is completely antagonized by P4. As with E2, P4 leads to an increase in uterine AHR levels, especially in the endometrial epithelium despite the decrease in corresponding mRNA levels. This indicates a complex gene-specific regulatory network involving E2, P4 and possibly AHR itself to maintain all components of the AHR signalling cascade at the required levels during all stages of the oestrous cycle and pregnancy.
机译:多项研究表明,芳烃受体(AHR)在介导许多工业化学品的毒性中起重要作用,在女性生殖器官的生理学中起重要作用。这很可能使AHR和AHR信号传导途径的其他成分处于女性类固醇的控制之下。在先前的研究中,我们已经可以证明大鼠子宫中17β-雌二醇(E2)对AHR电池许多成员的调节作用。在这项研究中,我们探讨了孕酮(P4)在这种情况下的潜在作用。在比较方法中,使用假手术的动物除运载体动物,E2,黄体酮(P4)或两种激素的组合治疗3天后,除假手术动物外,我们可以证明除E2之外,P4也是调节大鼠子宫AHR信号的重要因素。 P4在子宫Ahr,Arnt和Arnt2 mRNA水平上具有类似于E2的作用,导致这些基因的下调,而E2介导的关键AHR反应基因Cyp1a1,Gsta2和Ugt1的下调被P4完全拮抗。与E2一样,尽管相应的mRNA水平降低,P4也会导致子宫AHR水平升高,尤其是子宫内膜上皮细胞。这表明复杂的基因特异性调控网络涉及E2,P4以及可能的AHR本身,以在发情周期和妊娠的所有阶段将AHR信号传导级联的所有组件维持在所需水平。

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