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促分泌素对仓鼠克隆β细胞系HIT-T15在不同细胞外钙离子浓度下细胞溶质游离钙离子及胰岛素释放的影响

Effect of secretagogues on cytosolic free Ca2+ and insulin release at different extracellular Ca2+ concentrations in the hamster clonal beta-cell line HIT-T15.

作者信息

Hughes S J, Chalk J G, Ashcroft S J

机构信息

Nuffield Department of Clinical Biochemistry, John Radcliffe Hospital, Headington, Oxford, U.K.

出版信息

Mol Cell Endocrinol. 1989 Aug;65(1-2):35-41. doi: 10.1016/0303-7207(89)90162-7.

Abstract

We have examined the relationship between extracellular Ca2+, cytosolic free Ca2+ and insulin release in the clonal beta-cell line HIT-T15. Glucose-stimulated insulin release was dependent on the extracellular Ca2+ concentration in a dose-related manner; the threshold medium Ca2+ concentration for glucose-stimulated insulin release was 0.5 mM. Both forskolin and 12-O-tetradecanoylphorbol 13-acetate (TPA) increased insulin release in the presence of glucose at all extracellular Ca2+ concentration tested (0.1-2.5 mM) but not in the absence of Ca2+. Thus, the threshold medium Ca2+ concentration for glucose-stimulated insulin release was reduced to 0.1 mM by forskolin or TPA. Step-wise increases in the medium Ca2+ concentration in the presence of an initiator of insulin release resulted in a dose-related increase in cytosolic free Ca2+. In the presence of 10 mM glucose, cytosolic free Ca2+ in HIT cells was increased from 60 +/- 5 nM in Ca2+-free medium to 290 +/- 46 nM in medium containing 2.5 mM Ca2+. The effects of increasing extracellular Ca2+ in the presence of 40 mM K+ were similar but considerably more pronounced. Inclusion of either TPA or forskolin in the incubation medium had no significant effect on the steady-state cytosolic free Ca2+ levels in the absence of glucose but in the presence of 10 mM glucose forskolin caused modest (11-18%) increases in steady-state cytosolic free Ca2+ levels at extracellular Ca2+ concentrations of 0.25 mM or above. In contrast, in the presence of glucose TPA significantly reduced the steady-state levels of cytosolic free Ca2+ by 17-21% at extracellular Ca2+ concentrations of 0.25 mM or above. These data provide further evidence that insulin release mediated by activation of beta-cell protein kinases involves primarily an increase in sensitivity of the secretory system to intracellular Ca2+.

摘要

我们研究了克隆β细胞系HIT-T15中细胞外Ca2+、胞质游离Ca2+与胰岛素释放之间的关系。葡萄糖刺激的胰岛素释放以剂量相关的方式依赖于细胞外Ca2+浓度;葡萄糖刺激胰岛素释放的阈值培养基Ca2+浓度为0.5 mM。在所有测试的细胞外Ca2+浓度(0.1 - 2.5 mM)下,福斯可林和12 - O - 十四烷酰佛波醇13 - 乙酸酯(TPA)在有葡萄糖存在时均能增加胰岛素释放,但在无Ca2+时则不能。因此,福斯可林或TPA可将葡萄糖刺激胰岛素释放的阈值培养基Ca2+浓度降低至0.1 mM。在存在胰岛素释放启动剂的情况下,培养基中Ca2+浓度的逐步增加导致胞质游离Ca2+呈剂量相关增加。在10 mM葡萄糖存在下,HIT细胞中的胞质游离Ca2+从无Ca2+培养基中的60±5 nM增加到含2.5 mM Ca2+培养基中的290±46 nM。在40 mM K+存在下增加细胞外Ca2+的效果相似,但更为显著。在孵育培养基中加入TPA或福斯可林对无葡萄糖时的稳态胞质游离Ca2+水平无显著影响,但在10 mM葡萄糖存在下,福斯可林在细胞外Ca2+浓度为0.25 mM或更高时会使稳态胞质游离Ca2+水平适度增加(11 - 18%)。相反,在葡萄糖存在下,TPA在细胞外Ca2+浓度为0.25 mM或更高时会使胞质游离Ca2+的稳态水平显著降低17 - 21%。这些数据进一步证明,由β细胞蛋白激酶激活介导的胰岛素释放主要涉及分泌系统对细胞内Ca2+敏感性的增加。

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