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胰岛代谢、三磷酸腺苷含量与胰岛素释放之间的相互关系。

Interrelationship of islet metabolism, adenosine triphosphate content and insulin release.

作者信息

Ashcroft S J, Weerasinghe L C, Randle P J

出版信息

Biochem J. 1973 Feb;132(2):223-31. doi: 10.1042/bj1320223.

Abstract

The oxidation of some exogenous substrates and their effects on ATP content and insulin release in mouse pancreatic islets were measured. The ATP concentration of islets incubated without exogenous substrate shows a gradual decrease, which can be prevented by glucose or mannose (20mm) or leucine (2.5mm); d-glyceraldehyde (5mm) is as effective as glucose (5mm); fructose or N-acetylglucosamine (20mm), pyruvate (10mm) and dl-3-hydroxybutyrate (2mm) are less effective; galactose (20mm), acetate (10mm), octanoate (2mm) and succinate (10mm) have no ATP-maintaining ability. Islets oxidize glucose, mannose, glyceraldehyde, leucine and, less readily, N-acetylglucosamine and glucosamine; galactose, however, is poorly metabolized. Mannoheptulose inhibits the oxidation of glucose but not of glyceraldehyde. Insulin release, measured over a 2h incubation, is stimulated by glucose, mannose, leucine, glyceraldehyde or glucosamine but not by fructose or N-acetylglucosamine. The latter, however, potentiates the effects of glucose or glyceraldehyde (5mm) or leucine (2.5mm) on release; the potentiating effects are inhibited by mannoheptulose, which also blocks glucose-, but not glyceraldehyde- or leucine-stimulated release. In the presence of glucose (20mm), metabolic inhibitors depress insulin release and islet ATP content in parallel. However, rates of insulin release and ATP content measured after incubation with various combinations of exogenous substrates do not appear to be correlated. Sulphonylureas stimulate insulin release but decrease islet ATP concentrations. These results provide further evidence of a close association between the metabolic activity of exogenous substrates and their ability to initiate insulin release. Glucoreceptor models are formulated in the light of these observations and discussed.

摘要

测定了一些外源性底物的氧化作用及其对小鼠胰岛中ATP含量和胰岛素释放的影响。在没有外源性底物的情况下孵育的胰岛,其ATP浓度呈逐渐下降趋势,而葡萄糖或甘露糖(20mmol/L)或亮氨酸(2.5mmol/L)可阻止这种下降;d-甘油醛(5mmol/L)与葡萄糖(5mmol/L)的效果相同;果糖或N-乙酰葡糖胺(20mmol/L)、丙酮酸(10mmol/L)和dl-3-羟基丁酸(2mmol/L)的效果较差;半乳糖(20mmol/L)、乙酸盐(10mmol/L)、辛酸盐(2mmol/L)和琥珀酸盐(10mmol/L)没有维持ATP的能力。胰岛可氧化葡萄糖、甘露糖、甘油醛、亮氨酸,较难氧化N-乙酰葡糖胺和葡糖胺;然而,半乳糖的代谢较差。甘露庚酮糖抑制葡萄糖的氧化,但不抑制甘油醛的氧化。在2小时的孵育过程中测定胰岛素释放,发现葡萄糖、甘露糖、亮氨酸、甘油醛或葡糖胺可刺激胰岛素释放,而果糖或N-乙酰葡糖胺则不能。然而,后者可增强葡萄糖或甘油醛(5mmol/L)或亮氨酸(2.5mmol/L)对释放的作用;这种增强作用被甘露庚酮糖抑制,甘露庚酮糖也可阻断葡萄糖刺激的释放,但不阻断甘油醛或亮氨酸刺激的释放。在存在葡萄糖(20mmol/L)的情况下,代谢抑制剂会同时降低胰岛素释放和胰岛ATP含量。然而,用各种外源性底物组合孵育后测得的胰岛素释放速率和ATP含量似乎没有相关性。磺脲类药物刺激胰岛素释放,但会降低胰岛ATP浓度。这些结果进一步证明了外源性底物的代谢活性与其启动胰岛素释放的能力之间存在密切关联。根据这些观察结果构建并讨论了葡萄糖受体模型。

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