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Feminization imprinted by developmental growth hormone

机译:由发育生长激素印记的女性化

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Previously, we identified early developmental exposure to growth hormone (GH) as the requisite organizer responsible for programming the masculinization of the hepatic cytochromes P450 (CYP)-dependent drug metabolizing enzymes (Das et al., 2014, 2017). In spite of the generally held dogma that mammalian feminization requires no hormonal imprinting, numerous reports that the sex-dependent regulation and expression of hepatic CYPs in females are permanent and irreversible would suggest otherwise. Consequently, we selectively blocked GH secretion in a cohort of newborn female rats, some of whom received concurrent GH replacement or GH releasing factor. As adults, the feminine circulating GH profile was restored in the treated animals. Two categories of CYPs were measured. The principal and basically female specific CYP2C12 and CYP2C7; both completely and solely dependent on the adult feminine continuous GH profile for expression, and the female pre-dominant CYP2C6 and CYP2E1 whose expression is maximum in the absence of plasma GH, suppressed by the feminine GH profile but more so by the masculine episodic GH profile. Our findings indicate that early developmental exposure to GH imprints the inchoate CYP2C12 and CYP2C7 in the differentiating liver to be solely dependent on the feminine GH profile for expression in the adult female. In contrast, adult expression of CYP2C6 and CYP2E1 in the female rat appears to require no GH imprinting.
机译:以前,我们将早期发育暴露于生长激素(GH)作为负责编程肝细胞色素P450(CYP) - 依赖性药物代谢酶的阳像化(Das等,2014,2017)的必要组织者。尽管哺乳动物女性化不需要荷尔蒙印记的普遍持有的教条,但许多报告称,女性的性别依赖性调节和肝细胞癌的表达是永久性的,不可逆转的表明另有建议。因此,我们选择性地阻止了新生女性大鼠队列中的GH分泌物,其中一些人接受并发GH替换或GH发布因子。作为成年人,在治疗的动物中恢复了女性循环GH型材。测量了两类Cyps。主要和基本上女性特异性CYP2C12和CYP2C7;完全且完全依赖于成年女性连续GH谱的表达,以及在没有等离子体GH没有等离子体GH的情况下最大的雌性前显性CYP2C6和CYP2E1,由女性GH剖面抑制,但是MASSULINE EPISODIC GH型材。我们的研究结果表明,早期发育暴露于GH印记在差异肝脏中的Inthoate Cyp2C12和Cyp2C7,以完全依赖于女性女性在成年女性中表达的女性GH型材。相反,雌性大鼠中CYP2C6和CYP2E1的成人表达似乎不需要GH印迹。

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