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胰岛素及胰岛素样生长因子-I对大鼠胰腺β细胞分泌活性的直接作用

Direct effect of insulin and insulin-like growth factor-I on the secretory activity of rat pancreatic beta cells.

作者信息

Van Schravendijk C F, Heylen L, Van den Brande J L, Pipeleers D G

机构信息

Department of Metabolism and Endocrinology, Vrije Universiteit Brussel, Belgium.

出版信息

Diabetologia. 1990 Nov;33(11):649-53. doi: 10.1007/BF00400565.

Abstract

Purified pancreatic Beta cells were labelled with 3H-tyrosine before studying their secretory activity in perifusion. At 1.4 mmol/l glucose, the cells released similar fractions (0.01% per min) of their contents in preformed and in newly formed insulin. At 20 mmol/l glucose plus 10(-8) mol/l glucagon, these fractional release rates increased by 16 and 40-fold respectively. The preferential release of newly synthesized as compared to stored insulin is attributable to a heterogeneity in individual cell responses. The secretory responsiveness to glucose plus glucagon was completely suppressed by 10(-7) mol/l clonidine. Insulin induced a 20% reduction at 10(-6) mol/l, but remained without effect at 10(-7) mol/l. Insulin-like growth factor-I provoked a 30% decrease at 5.10(-9) mol/l. It is concluded that the type-I insulin-like growth factor receptors on pancreatic Beta cells mediate a suppressive action on the insulin release process. Their high affinity for insulin-like growth factor-I allows physiologic levels of this peptide to participate in the regulation of insulin release. Their low affinity for insulin provides the basis for a minor feedback action by this hormone at concentrations exceeding the normal circulating levels.

摘要

在研究纯化的胰岛β细胞在灌流中的分泌活性之前,先用³H - 酪氨酸对其进行标记。在1.4 mmol/L葡萄糖浓度下,细胞以相似的比例(每分钟0.01%)释放预先形成的胰岛素和新合成的胰岛素。在20 mmol/L葡萄糖加10⁻⁸mol/L胰高血糖素的条件下,这些释放比例分别增加了16倍和40倍。与储存的胰岛素相比,新合成的胰岛素优先释放归因于单个细胞反应的异质性。10⁻⁷mol/L可乐定可完全抑制对葡萄糖加胰高血糖素的分泌反应。胰岛素在10⁻⁶mol/L时可使分泌反应降低20%,但在10⁻⁷mol/L时无作用。胰岛素样生长因子 - I在5×10⁻⁹mol/L时可使分泌反应降低30%。结论是胰岛β细胞上的I型胰岛素样生长因子受体介导了对胰岛素释放过程的抑制作用。它们对胰岛素样生长因子 - I的高亲和力使该肽的生理水平能够参与胰岛素释放的调节。它们对胰岛素的低亲和力为该激素在超过正常循环水平的浓度下产生的轻微反馈作用提供了基础。

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