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胰岛素对甲状旁腺激素合成、细胞内降解及分泌的影响。

Effects of insulin on the synthesis, intracellular degradation, and secretion of parathormone.

作者信息

Hinton D A, MacGregor R R

机构信息

Department of Anatomy and Cell Biology, University of Kansas Medical Center, Kansas City 66103.

出版信息

Endocrinology. 1991 Jan;128(1):488-95. doi: 10.1210/endo-128-1-488.

Abstract

Bovine parathyroid organoids were maintained for up to 12 days of culture in the presence or absence of insulin. Insulin-treated organoids secreted more PTH and secretory protein-I (SP-I) than did untreated organoids at both 1.4 and 1.8 mM Ca, concentrations chosen to promote partially elevated and suppressed secretion rates, respectively. The insulin effect was dose dependent and reversible. To determine whether insulin might increase secretion by reducing degradation of cellular PTH, its effects on several parameters related to degradative processes were examined. Compared to control cultures maintained at either 1.4 or 1.8 mM Ca, insulin did not induce changes in the relative levels of intact hormone and COOH-terminal peptide fragments secreted into culture medium, nor did it decrease the total cellular levels of three lysosomal enzymes or mute the effects of 3-methyladenine (an agent that decreases formation of autophagosomes) to increase PTH secretion. Thus, insulin did not appear to increase PTH secretion by reducing the latter's cellular degradation. Synthesis of total proteins and of the secreted proteins SP-I and PTH was examined using short incubations of control and insulin-treated organoids with [3H] leucine. Incorporation of 3H into total acid-precipitable proteins was not elevated in insulin-treated organoids; that into PTH/pro-PTH and SP-I, however, was significantly greater in insulin-treated than in control organoids. The results suggested that the insulin-mediated increase in PTH and SP-I secretion is largely due to its regulation of PTH and SP-I biosynthesis.

摘要

牛甲状旁腺类器官在有或无胰岛素的情况下培养长达12天。在1.4 mM和1.8 mM钙浓度下,胰岛素处理的类器官比未处理的类器官分泌更多的甲状旁腺激素(PTH)和分泌蛋白I(SP-I),这两种钙浓度分别用于促进部分升高和抑制分泌率。胰岛素的作用是剂量依赖性的且可逆。为了确定胰岛素是否可能通过减少细胞内PTH的降解来增加分泌,研究了其对与降解过程相关的几个参数的影响。与在1.4 mM或1.8 mM钙浓度下培养的对照培养物相比,胰岛素并未引起分泌到培养基中的完整激素和COOH末端肽片段相对水平的变化,也未降低三种溶酶体酶的总细胞水平,也未消除3-甲基腺嘌呤(一种减少自噬体形成的试剂)增加PTH分泌的作用。因此,胰岛素似乎并未通过减少PTH的细胞降解来增加其分泌。使用对照和胰岛素处理的类器官与[3H]亮氨酸进行短时间孵育,检测总蛋白以及分泌蛋白SP-I和PTH的合成。胰岛素处理的类器官中3H掺入总酸沉淀蛋白的量并未增加;然而,胰岛素处理的类器官中3H掺入PTH/前PTH和SP-I的量显著高于对照类器官。结果表明,胰岛素介导的PTH和SP-I分泌增加主要归因于其对PTH和SP-I生物合成的调节。

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