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生长激素和胰岛素与遗传性侏儒小鼠分离肝细胞的结合

Growth hormone and insulin binding to isolated hepatocytes in the genetically dwarf mouse.

作者信息

Fouchereau-Peron M, Broer Y, Rosselin G

出版信息

Biochim Biophys Acta. 1980 Sep 1;631(3):451-62. doi: 10.1016/0304-4165(80)90021-5.

Abstract

The interaction of growth hormone with its specific receptors in dwarf mice was investigated. (1) The interaction of 125I-labeled human growth hormone with isolated mouse liver cells is a specific, time-dependent and saturable process. Hepataocytes of male and female dw/dw mice bound only 10-20% as much growth hormone per unit of cell surface area as those of their litter mates. Scatchard analysis suggested that this decrease in binding was due to a decreased number of receptor sites in th liver cell of the dwarf mouse. (2) In contrast to the marked decrease in growth hormone receptors, the binding of insulin is higher in dwarf mice than in litter mates, at low hormone concentration. (3) Competition and stoichiometric studies indicate that growth hormone and prolactin bind to the same type of binding site in female and male mouse hepatocytes. These results indicate that dwarfism in this animal was associated with a loss in the number of growth hormone binding sites. The decrease in growth hormone receptors and the increase in insulin receptors correlate well with the respective biological activity of these two hormones.

摘要

研究了生长激素与其在侏儒小鼠中的特异性受体的相互作用。(1)125I标记的人生长激素与分离的小鼠肝细胞的相互作用是一个特异性、时间依赖性和可饱和的过程。雄性和雌性dw/dw小鼠的肝细胞每单位细胞表面积结合的生长激素仅为其同窝小鼠的10%-20%。Scatchard分析表明,这种结合减少是由于侏儒小鼠肝细胞中受体位点数量减少所致。(2)与生长激素受体的显著减少相反,在低激素浓度下,侏儒小鼠中胰岛素的结合高于同窝小鼠。(3)竞争和化学计量学研究表明,生长激素和催乳素在雌性和雄性小鼠肝细胞中结合到同一类型的结合位点。这些结果表明,这种动物的侏儒症与生长激素结合位点数量的丧失有关。生长激素受体的减少和胰岛素受体的增加与这两种激素各自的生物学活性密切相关。

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