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雌激素通过一种独立于垂体蛋白合成的机制刺激催乳素基因转录。

Estrogen stimulates prolactin gene transcription by a mechanism independent of pituitary protein synthesis.

作者信息

Shull J D, Gorski J

出版信息

Endocrinology. 1984 May;114(5):1550-7. doi: 10.1210/endo-114-5-1550.

Abstract

We have used an in vitro nuclear transcription system to investigate the mechanisms through which 17 beta-estradiol regulates PRL gene expression in the rat pituitary. A single injection of this estrogen stimulated the rate of PRL RNA synthesis in nuclei isolated from male rats within 30 min of treatment, and this stimulated rate of PRL RNA synthesis was observed for at least 48 h after injection. In contrast, estrogen treatment had little effect on the rate of GH RNA synthesis. Cycloheximide, at a dose sufficient to inhibit pituitary protein synthesis by greater than 80%, did not block this estradiol-mediated stimulation of PRL RNA synthesis through at least the first 8 h after hormone treatment. Estradiol treatment also resulted in a rapid transformation of the pituitary estrogen receptors from the cytosolic to the nuclear form. However, the level of receptor in the nuclear form peaked within 1 h and had returned to near the control value within 6 h of hormone injection. These studies suggest that 17 beta-estradiol regulates PRL gene transcription through a mechanism independent of pituitary protein synthesis. In addition, the rates of PRL RNA synthesis over the time course examined were not correlated with the percentage of the pituitary estrogen receptor population existing in the nuclear form.

摘要

我们使用了一种体外核转录系统来研究17β-雌二醇调节大鼠垂体中PRL基因表达的机制。单次注射这种雌激素在处理后30分钟内刺激了从雄性大鼠分离的细胞核中PRL RNA的合成速率,并且在注射后至少48小时内都观察到了这种PRL RNA合成速率的刺激。相比之下,雌激素处理对GH RNA合成速率几乎没有影响。环己酰亚胺以足以抑制垂体蛋白合成超过80%的剂量处理,在激素处理后的至少前8小时内并未阻断这种雌二醇介导的PRL RNA合成刺激。雌二醇处理还导致垂体雌激素受体迅速从胞质形式转变为核形式。然而,核形式的受体水平在1小时内达到峰值,并在激素注射后6小时内恢复到接近对照值。这些研究表明,17β-雌二醇通过一种独立于垂体蛋白合成的机制调节PRL基因转录。此外,在所研究的时间进程中PRL RNA合成速率与以核形式存在的垂体雌激素受体群体的百分比无关。

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