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胰岛素调节垂体细胞中催乳素的分泌及信使核糖核酸水平。

Insulin regulates prolactin secretion and messenger ribonucleic acid levels in pituitary cells.

作者信息

Prager D, Yamashita S, Melmed S

机构信息

Department of Medicine, Cedars-Sinai Medical Center, University of California School of Medicine, Los Angeles 90048.

出版信息

Endocrinology. 1988 Jun;122(6):2946-52. doi: 10.1210/endo-122-6-2946.

Abstract

The regulation of PRL production in GH3 rat pituitary tumor cells and normal rat pituitary cells exposed to insulin was studied. Cells were treated with semisynthetic human insulin for up to 5 days. Insulin (0.7 nM) stimulated PRL production by 30%, and cortisol (100 nM) suppressed it by 80% in GH3 cells. Insulin (3.5 nM) partially blocked the suppression of PRL secretion induced by up to 100 nM cortisol. Equimolar doses of insulin-like growth factor I failed to consistently stimulate either basal PRL secretion into the medium or cortisol-suppressed PRL in GH3 cells. A 65 nM concentration of insulin-like growth factor I was required to stimulate basal PRL secretion in GH3 cells. Relative levels of PRL mRNA sequences in both GH3 cells and normal rat pituitary cells were stimulated by insulin. When cells were incubated with cortisol (10 nM), PRL mRNA levels were suppressed to 40% of control values. Simultaneous incubation of cells with insulin (3.5 nM) partially reversed the cortisol-induced suppression of PRL mRNA to 60% of control values. The results show that insulin antagonizes cortisol-induced suppression of PRL. Physiological doses of insulin stimulate PRL production and PRL mRNA levels, suggesting a direct effect of insulin on either PRL gene transcription or stabilization of PRL mRNA in these cells.

摘要

研究了胰岛素对GH3大鼠垂体瘤细胞和正常大鼠垂体细胞中催乳素(PRL)分泌的调节作用。细胞用半合成人胰岛素处理长达5天。在GH3细胞中,胰岛素(0.7 nM)可使PRL分泌增加30%,而皮质醇(100 nM)可使其分泌减少80%。胰岛素(3.5 nM)可部分阻断高达100 nM皮质醇诱导的PRL分泌抑制。等摩尔剂量的胰岛素样生长因子I未能持续刺激GH3细胞中基础PRL分泌到培养基中或皮质醇抑制的PRL分泌。需要65 nM浓度的胰岛素样生长因子I来刺激GH3细胞中的基础PRL分泌。胰岛素可刺激GH3细胞和正常大鼠垂体细胞中PRL mRNA序列的相对水平。当细胞与皮质醇(10 nM)一起孵育时,PRL mRNA水平被抑制至对照值的40%。细胞与胰岛素(3.5 nM)同时孵育可将皮质醇诱导的PRL mRNA抑制部分逆转至对照值的60%。结果表明,胰岛素可拮抗皮质醇诱导的PRL分泌抑制。生理剂量的胰岛素可刺激PRL分泌和PRL mRNA水平,提示胰岛素对这些细胞中PRL基因转录或PRL mRNA稳定性有直接作用。

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