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子宫催产素基因表达。II. 外源性甾体给药诱导

Uterine oxytocin gene expression. II. Induction by exogenous steroid administration.

作者信息

Lefebvre D L, Farookhi R, Giaid A, Neculcea J, Zingg H H

机构信息

Laboratory of Molecular Endocrinology, Royal Victoria Hospital, Montreal, Quebec, Canada.

出版信息

Endocrinology. 1994 Jun;134(6):2562-6. doi: 10.1210/endo.134.6.8194483.

Abstract

As we have recently shown, the gene encoding the hypothalamic nonapeptide oxytocin (OT) is expressed in the rat endometrial epithelium during late pregnancy and the estrous phase of the estrous cycle. To investigate the role of ovarian steroids in the regulation of uterine OT gene expression, Silastic capsules containing estradiol or progesterone were implanted into immature ovariectomized rats. Exposure to estradiol alone for 2 days caused a significant rise in OT mRNA. Administration of progesterone alone was without effect. However, a strong synergism was observed when the two hormones were applied together; progesterone potentiated the effect of estradiol by a factor of 7. In animals treated with steroids for 4 days, the removal of either the estradiol or progesterone capsule after day 2 led to a decrease in the total amount of OT mRNA accumulation, implying that the continued action of both steroids was required to achieve maximal OT mRNA levels. Immunocytochemical analysis demonstrated that the main site of steroid-induced uterine OT gene expression is the endometrial epithelium, the same site where endogenously induced OT gene expression occurs at the end of pregnancy. The OT mRNA levels achieved after 4 days of treatment with both steroids were comparable to those achieved at estrus or during pseudopregnancy, but corresponded to less than 20% of the levels present in the uterus on day 21 of pregnancy. These data suggest that in the uterus, the synergistic action of ovarian steroids represents an important, but probably not exclusive, regulator of OT gene expression.

摘要

正如我们最近所表明的,编码下丘脑九肽催产素(OT)的基因在妊娠后期和发情周期的发情期在大鼠子宫内膜上皮中表达。为了研究卵巢类固醇在子宫OT基因表达调控中的作用,将含有雌二醇或孕酮的硅橡胶胶囊植入未成熟卵巢切除的大鼠体内。单独暴露于雌二醇2天会导致OT mRNA显著升高。单独给予孕酮则没有效果。然而,当两种激素一起应用时观察到强烈的协同作用;孕酮使雌二醇的作用增强了7倍。在用类固醇处理4天的动物中,在第2天后移除雌二醇或孕酮胶囊会导致OT mRNA积累总量减少,这意味着两种类固醇的持续作用是达到最大OT mRNA水平所必需的。免疫细胞化学分析表明,类固醇诱导的子宫OT基因表达的主要部位是子宫内膜上皮,这与妊娠末期内源性诱导OT基因表达的部位相同。用两种类固醇处理4天后达到的OT mRNA水平与发情期或假孕期间达到的水平相当,但仅相当于妊娠第21天子宫中存在水平的不到20%。这些数据表明,在子宫中,卵巢类固醇的协同作用是OT基因表达的一个重要但可能不是唯一的调节因子。

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