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雌激素对垂体中c-fos表达的细胞特异性诱导。

Cell-specific induction of c-fos expression in the pituitary gland by estrogen.

作者信息

Allen D L, Mitchner N A, Uveges T E, Nephew K P, Khan S, Ben-Jonathan N

机构信息

Department of Cell Biology, Neurobiology, and Anatomy, University of Cincinnati School of Medicine, Ohio 45267-0521, USA.

出版信息

Endocrinology. 1997 May;138(5):2128-35. doi: 10.1210/endo.138.5.5101.

Abstract

Estrogens regulate many functions of pituitary lactotrophs, including PRL gene expression, release, storage, and cellular proliferation. The mechanism by which estrogens exert such a variety of functions is poorly understood. In the uterus, estrogens rapidly and transiently induce the expression of the immediate early genes c-fos and c-jun in specific cell types. The Fos/Jun proteins form the activating protein-1 (AP1) transcription factor that mediates ligand-activated cell proliferation, differentiation, and secretion. Here we used Fischer 344 (F344) rats that develop hyperprolactinemia and prolactinomas in response to estrogens. The objectives were to: 1) determine whether estrogen induces c-fos expression in the pituitary gland and identify the responsive cells; 2) compare the dynamics of c-fos induction in the pituitary and uterus; and 3) examine the temporal relationship between c-fos expression and PRL release. Ovariectomized F344 rats were injected with 1 microg estradiol and killed at different times thereafter. Pituitaries were subjected to in situ hybridization for c-fos and immunostaining for selected pituitary cells. Estradiol stimulated c-fos expression in lactotrophs and folliculo-stellate cells within the anterior lobe without affecting either the intermediate or neural lobes. In a second experiment, c-fos messenger RNA levels were measured by solution hybridization in anterior pituitaries and uteri from estradiol-treated rats. Trunk blood was analyzed for PRL by RIA. The estrogen-induced c-fos rise in the uterus was rapid, robust, and transient, whereas that in the anterior pituitary was delayed, lower, and sustained. The profile of serum PRL levels resembles that of c-fos induction in the anterior pituitary. We conclude that: 1) both lactotrophs and folliculo-stellate cells increase c-fos expression in response to estrogens; 2) induction of c-fos expression may mediate some estrogenic effects on PRL synthesis and release and lactotroph proliferation in F344 rats; and 3) the atypical dynamics of c-fos induction in the pituitary could be due to indirect effects of estrogens on PRL-regulating factors within the hypothalamo-pituitary complex as well as to pituitary-specific estrogen receptor isoforms, coactivators, or repressors.

摘要

雌激素调节垂体催乳素细胞的多种功能,包括催乳素(PRL)基因表达、释放、储存及细胞增殖。雌激素发挥这些多样功能的机制尚不清楚。在子宫中,雌激素能在特定细胞类型中快速且短暂地诱导即刻早期基因c-fos和c-jun的表达。Fos/Jun蛋白形成激活蛋白-1(AP1)转录因子,介导配体激活的细胞增殖、分化及分泌。在此,我们使用了对雌激素产生高催乳素血症和催乳素瘤的Fischer 344(F344)大鼠。目的是:1)确定雌激素是否诱导垂体中c-fos的表达并识别反应性细胞;2)比较垂体和子宫中c-fos诱导的动力学;3)研究c-fos表达与PRL释放之间的时间关系。切除卵巢的F344大鼠注射1微克雌二醇,并在此后不同时间处死。对垂体进行c-fos原位杂交及对选定垂体细胞进行免疫染色。雌二醇刺激前叶催乳素细胞和滤泡-星状细胞中c-fos的表达,而对中间叶或神经叶无影响。在第二个实验中,通过溶液杂交测量雌二醇处理大鼠的垂体前叶和子宫中c-fos信使核糖核酸水平。通过放射免疫分析法分析躯干血中的PRL。雌激素诱导子宫中c-fos升高迅速、强烈且短暂,而垂体前叶中的升高则延迟、较低且持续。血清PRL水平的变化趋势类似于垂体前叶中c-fos的诱导情况。我们得出结论:1)催乳素细胞和滤泡-星状细胞均会因雌激素而增加c-fos的表达;2)c-fos表达的诱导可能介导了雌激素对F344大鼠PRL合成、释放及催乳素细胞增殖的某些作用;3)垂体中c-fos诱导的非典型动力学可能是由于雌激素对下丘脑-垂体复合体中PRL调节因子的间接作用以及垂体特异性雌激素受体亚型、共激活因子或抑制因子所致。

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