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首页> 外文期刊>Journal of neurobiology >Progesterone receptor gene and protein expression in the anterior preoptic area and hypothalamus of defeminized rats.
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Progesterone receptor gene and protein expression in the anterior preoptic area and hypothalamus of defeminized rats.

机译:去女性大鼠的前视前区和下丘脑孕酮受体基因和蛋白表达

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摘要

Progesterone receptor (PR) plays an important role during sexual differentiation of the rat brain. The objective of the present study was to determine PR protein and gene expression pattern in preoptic-anterior hypothalamic area (POA-AHA) and hypothalamus (HYP), after estradiol or testosterone treatment during the postnatal critical period of sexual differentiation of the rat brain (defeminized animals). Three-day-old female rats were subcutaneously (s.c.) injected with a single dose of 17beta-estradiol (200 microg), or testosterone enanthate (200 microg), or vehicle (corn oil). POA-AHA and HYP were dissected 3 h, 24 h, and 14 days, as well as on the day of vaginal opening (VO) after treatments. Other animals, previously treated as above, were acutely injected with 17beta-estradiol (5 microg) on the day of VO; POA-AHA and HYP were obtained 3 h later. Total RNA was extracted and processed for semiquantitative RT-PCR and tissue slices were prepared for protein detection by immunohistochemistry. We observed that PR mRNA expression was increased in POA-AHA and HYP of the animals treated with estradiol or testosterone 3 hours after treatments, compared with the vehicle-treated control group. We also found a significant increase in PR mRNA and protein expression in POA-AHA and HYP on the day of VO in both estradiol and testosterone defeminized rats. Interestingly, the acute administration of estradiol on the day of VO (VO + E(2)) did not increase PR mRNA or protein expression in POA-AHA and HYP of either estradiol or testosterone defeminized animals, as opposed to the marked induction observed in the intact animals of the control group. The overall results suggest that estradiol and testosterone treatment during the postnatal critical period of sexual differentiation of the brain modifies the regulation of the PR mRNA and protein expression during early onset of maturity.
机译:孕酮受体(PR)在大鼠大脑的性别分化中起重要作用。本研究的目的是确定在出生后大鼠脑性分化关键时期进行雌二醇或睾丸激素治疗后,在视前前下丘脑区(POA-AHA)和下丘脑(HYP)中的PR蛋白和基因表达模式(去女性化的动物)。给三天大的雌性大鼠皮下注射(s.c.)单剂量的17β-雌二醇(200微克),睾丸酮庚酸酯(200微克)或赋形剂(玉米油)。在治疗后3小时,24小时和14天以及阴道开放(VO)当天解剖POA-AHA和HYP。在VO当天,对先前按上述方法治疗的其他动物急性注射17β-雌二醇(5微克)。 3小时后获得POA-AHA和HYP。提取总RNA并进行半定量RT-PCR处理,并准备组织切片用于通过免疫组织化学检测蛋白质。我们观察到,与媒介物处理的对照组相比,在处理3小时后用雌二醇或睾丸激素处理的动物的POA-AHA和HYP中PR mRNA表达增加。我们还发现雌二醇和睾丸激素脱女性大鼠的VO当天,POA-AHA和HYP中PR mRNA和蛋白表达显着增加。有趣的是,在VO(VO + E(2))那天急性给予雌二醇并没有增加雌二醇或睾丸激素脱女性动物的POA-AHA和HYP中PR mRNA或蛋白表达,与在OH中观察到的明显诱导相反。对照组的完整动物。总体结果表明,在脑部性分化的产后关键时期,雌二醇和睾丸激素的治疗​​会在成熟的早期发作时改变PR mRNA和蛋白表达的调节。

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