首页> 外文期刊>Molecular and Cellular Endocrinology >Development of a human stanniocalcin radioimmunoassay: serum and tissue hormone levels and pharmacokinetics in the rat.
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Development of a human stanniocalcin radioimmunoassay: serum and tissue hormone levels and pharmacokinetics in the rat.

机译:人锡钙钙素放射免疫分析的发展:大鼠血清和组织激素水平及药代动力学。

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摘要

Stanniocalcin (STC) is a polypeptide hormone that was first discovered in fish and recently identified in humans and other mammals. In fish STC is produced by one gland, circulates freely in the blood and plays an integral role in mineral homeostasis. In mammals, STC is produced in a number of different tissues and serves a variety of different functions. In kidney, STC regulates phosphate reabsorption by proximal tubule cells, whereas in ovary it appears to be involved in steroid hormone synthesis. However there is no information on circulating levels of STC in mammals or the regulation of its secretion. In this report we have developed a radioimmunoassay (RIA) for human STC. The RIA was validated for measuring tissue hormone levels. However human and other mammalian sera were completely devoid of immunoreactive STC (irSTC). To explore the possibility that mammalian STC might have a short half-life pharmacokinetic analysis was carried out in rats. STC pharmacokinetics were best described by a two compartment model where the distribution phase (t1/2(alpha)) equaled 1 min and the elimination phase (t1/2(beta)) was 60 min. However the STC in the elimination phase no longer crossreacted in the RIA indicating it had undergone substantial chemical modification, which could explain our inability to detect irSTC in mammalian sera. When we compared the pharmacokinetics of human and fish STC in mammalian and fish models the human hormone was always eliminated faster, indicating that human STC has unique structural properties. There also appears to be a unique clearance mechanism for STC in mammals. Hence there are major differences in the delivery and biology of mammalian STC. Unlike fishes, mammalian STC does not normally circulate in the blood and functions instead as a local mediator of cell function. Future studies will no doubt show that this has had important ramifications on function as well.
机译:锡钙素(STC)是一种多肽激素,最早在鱼类中发现,最近在人类和其他哺乳动物中得到鉴定。在鱼类中,STC由一个腺体产生,在血液中自由循环,在矿物质体内平衡中起着不可或缺的作用。在哺乳动物中,STC在许多不同的组织中产生,并具有多种不同的功能。在肾脏中,STC调节近端肾小管细胞对磷酸盐的重吸收,而在卵巢中,它似乎参与类固醇激素的合成。然而,没有关于哺乳动物中STC的循环水平或其分泌调节的信息。在本报告中,我们开发了用于人类STC的放射免疫分析(RIA)。 RIA已验证可用于测量组织激素水平。但是,人类和其他哺乳动物的血清完全没有免疫反应性STC(irSTC)。为了探索哺乳动物STC可能具有短的半衰期药代动力学分析的可能性,在大鼠中进行。 STC药代动力学最好用两室模型来描述,其中分布阶段(t1 /2α)等于1分钟,消除阶段(t1 /2β)为60分钟。但是,处于消除阶段的STC在RIA中不再发生交叉反应,这表明它已经进行了重大的化学修饰,这可以解释我们无法在哺乳动物血清中检测到irSTC。当我们在哺乳动物和鱼类模型中比较人和鱼STC的药代动力学时,总是会更快地消除人的激素,这表明人STC具有独特的结构特性。在哺乳动物中,STC似乎也有独特的清除机制。因此,在哺乳动物STC的递送和生物学上存在主要差异。与鱼类不同,哺乳动物的STC通常不会在血液中循环,而是充当细胞功能的局部介体。毫无疑问,未来的研究表明,这也对功能产生了重要影响。

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