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培养肝细胞中纤维蛋白原合成的激素调节

Hormonal regulation of fibrinogen synthesis in cultured hepatocytes.

作者信息

Grieninger G, Plant P W, Liang T J, Kalb R G, Amrani D, Mosesson M W, Hertzberg K M, Pindyck J

出版信息

Ann N Y Acad Sci. 1983 Jun 27;408:469-89. doi: 10.1111/j.1749-6632.1983.tb23267.x.

Abstract

Most of what was originally known of the effects of hormones on fibrinogen synthesis was based, as noted above, on experiments involving surgical removal of endocrine glands. Some caution should be exercised when using such in vivo experiments to derive the hormonal requirements of fibrinogen synthesis, however, since multiple hormonal alterations often occur in these animals. The development of a variety of ex vivo systems has allowed investigators to more carefully control the hepatocellular environment. The work of several laboratories, including our own, has now made it clear that hormones and other agents directly stimulate hepatocellular synthesis of fibrinogen. From the studies summarized here, using chick embryo hepatocytes as a model, several generalizations emerge: Fibrinogen synthesis may be considered to be a "constitutive" liver function, since hepatocytes cultured without serum, hormones or other macromolecular supplements synthesize this protein at a basal rate for several days. Addition of certain hormones (e.g. T3, dexamethasone, insulin), individually and in physiological concentrations, elicits an increase in fibrinogen production, varying with each agent in onset, dose, minimum exposure required and accompanying effects on the synthesis of other plasma proteins. Glucocorticoids and thyroid hormones are similar in the selectivity of their stimulation (neither affects albumin or transferrin synthesis) but differ in that thyroid hormones need to be present for just a short "triggering" period. The stimulation of fibrinogen synthesis by insulin occurs only following prolonged exposure to concentrations 10-times higher than the very low doses to which albumin synthesis responds rapidly.

摘要

如前所述,最初关于激素对纤维蛋白原合成影响的大部分认识是基于涉及手术切除内分泌腺的实验。然而,在使用此类体内实验来推导纤维蛋白原合成的激素需求时应谨慎,因为这些动物中经常会出现多种激素变化。各种体外系统的发展使研究人员能够更仔细地控制肝细胞环境。包括我们自己实验室在内的几个实验室的工作现已明确表明,激素和其他因子可直接刺激肝细胞合成纤维蛋白原。从这里总结的以鸡胚肝细胞为模型的研究中,可以得出几个一般性结论:纤维蛋白原合成可被视为一种“组成性”肝功能,因为在无血清、激素或其他大分子补充物的情况下培养的肝细胞会以基础速率合成这种蛋白质达数天之久。单独添加某些激素(如T3、地塞米松、胰岛素)并以生理浓度添加,会引起纤维蛋白原产量增加,每种激素在起效时间、剂量、所需最短暴露时间以及对其他血浆蛋白合成的伴随影响方面各不相同。糖皮质激素和甲状腺激素在刺激的选择性方面相似(两者均不影响白蛋白或转铁蛋白合成),但不同之处在于甲状腺激素只需存在较短的“触发”期。胰岛素对纤维蛋白原合成的刺激仅在长时间暴露于比白蛋白合成快速响应的极低剂量高10倍的浓度后才会发生。

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