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胰岛中D-葡萄糖异头物代谢的进一步研究。

Further studies on the metabolism of D-glucose anomers in pancreatic islets.

作者信息

Idahl L A, Rahemtulla F, Sehlin J, Täljedal I B

出版信息

Diabetes. 1976 May;25(5):450-8. doi: 10.2337/diab.25.5.450.

Abstract

The alpha and beta anomers of commercially available D-(5-3H) glucose were separated by miniaturized Hudson-Dale procedures based on precipitation with acetic acid. Reflectometric measurements of the reactivity with matrix-bound glucose oxidase showed that the preparations were about 90 per cent pure with respect to anomeric composition. Nonradioactive anomers separated by the same procedures were analyzed by optic polarimetry and gas chromatography. The preparations were about 90 per cent pure with respect to anomeric composition and produced no peaks but D-glucose on trimethylsilylation and chromatography. Microdissected pancreatic islets of noninbred ob/ob-mice exhibited a linear production of 3H2O for three to nine minutes when incubated with 6 mM alpha-D-(5-3H) glucose, beta-D-(5-3H) glucose, or D-(5-3H) glucose in anomeric equilibrium; the three glucose preparations did not differ in their rate of conversion to 3H2O. The rate of 3H2O production increased with glucose concentration (3-21 mM) during incubations for three minutes and, again, there was no evidence for the metabolic activity's being dependent on the anomeric composition of the labeled sugar. When microdissected islets were perifused without glucose and suddenly exposed to 5-6 mM alpha-D-glucose or beta-D-glucose, the concentration of glucose-6-phosphate rose within five minutes and did not differ significantly between experiments with alpha-D-glucose and beta-D-glucose. In the same perifusion experiments, only alpha-D-glucose caused a pronounced stimulation of insulin secretion, the difference from beta-D-glucose being significant. The results indicate that the recognition of glucose as an insulin secretagogue does not only involve metabolism by glucose-6-phosphate. The possible roles of the sorbitol pathway and of hypothetical regulatory sites for the glucose molecule ("receptors") are briefly discussed.

摘要

基于用乙酸沉淀的小型化哈德森-戴尔程序,分离市售D-(5-³H)葡萄糖的α和β异头物。对与基质结合的葡萄糖氧化酶反应性的反射测量表明,就异头物组成而言,制剂纯度约为90%。通过相同程序分离的非放射性异头物通过旋光偏振法和气相色谱法进行分析。就异头物组成而言,制剂纯度约为90%,在三甲基硅烷化和色谱分析时除了D-葡萄糖外没有产生其他峰。当用6 mMα-D-(5-³H)葡萄糖、β-D-(5-³H)葡萄糖或处于异头物平衡的D-(5-³H)葡萄糖孵育时,非近交ob/ob小鼠的显微解剖胰岛在三到九分钟内呈现³H₂O的线性产生;三种葡萄糖制剂转化为³H₂O的速率没有差异。在三分钟的孵育过程中,³H₂O的产生速率随葡萄糖浓度(3-21 mM)增加,同样,没有证据表明代谢活性依赖于标记糖的异头物组成。当显微解剖的胰岛在无葡萄糖的情况下进行灌流并突然暴露于5-6 mMα-D-葡萄糖或β-D-葡萄糖时,葡萄糖-6-磷酸的浓度在五分钟内升高,α-D-葡萄糖和β-D-葡萄糖的实验之间没有显著差异。在相同的灌流实验中,只有α-D-葡萄糖引起胰岛素分泌的显著刺激,与β-D-葡萄糖的差异显著。结果表明,将葡萄糖识别为胰岛素促分泌剂不仅涉及通过葡萄糖-6-磷酸的代谢。简要讨论了山梨醇途径和葡萄糖分子假设调节位点(“受体”)的可能作用。

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