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S 21403对不同葡萄糖浓度下分离的大鼠胰腺激素分泌的影响。

Effects of S 21403 on hormone secretion from isolated rat pancreas at different glucose concentrations.

作者信息

Gregorio Franco, Ambrosi Franca, Boemi Massimo, Carle Flavia, Filipponi Paolo

机构信息

Anti-Diabetic Unit, Medical Department E. Profili General Hospital, 60044 Fabriano, AN, Italy.

出版信息

Eur J Pharmacol. 2002 Dec 5;456(1-3):141-7. doi: 10.1016/s0014-2999(02)02620-1.

Abstract

We investigated the in vitro effects of therapeutical concentrations of S 21403 (a succinic acid derivative also known as KAD 1229 and mitiglinide) on insulin and glucagon secretion during a metabolic stimulus (glucose rising from 5 to 8.33 mM) or at a stable 2.22 mM glucose using the isolated perfused rat pancreas model, and we compared them with the patterns of repaglinide and glibenclamide. Control perfusions were also performed. During 8.33 mM glucose, insulin release peaked to 339.12+/-22.87 microU/ml in controls. S 21403 enhanced insulin release (first peak 413.02+/-14.90 microU/ml; P<0.03 vs. controls, P=ns vs. repaglinide, P<0.005 vs. glibenclamide). Repaglinide increased glucose-induced first peak secretion to 409.33+/-20.05 microU/ml within the eighth minute (P<0.05 vs. controls, P<0.01 vs. glibenclamide). Glibenclamide did not affect the first phase of glucose-induced insulin release (peak of 338.41+/-29.79 microU/ml) but potentiated and delayed the second phase. No drug affected glucagon release. In conclusion, S 21403 induces a faster, more physiological pattern of insulin release than the other drugs we tested.

摘要

我们使用离体灌注大鼠胰腺模型,研究了治疗浓度的S 21403(一种琥珀酸衍生物,也称为KAD 1229和米格列奈)在代谢刺激(葡萄糖从5 mM升至8.33 mM)期间或在稳定的2.22 mM葡萄糖条件下对胰岛素和胰高血糖素分泌的体外影响,并将其与瑞格列奈和格列本脲的作用模式进行了比较。还进行了对照灌注。在8.33 mM葡萄糖期间,对照组胰岛素释放峰值达到339.12±22.87微单位/毫升。S 21403增强了胰岛素释放(第一个峰值为413.02±14.90微单位/毫升;与对照组相比P<0.03,与瑞格列奈相比P=无显著性差异,与格列本脲相比P<0.005)。瑞格列奈在第八分钟内将葡萄糖诱导的第一个峰值分泌增加到409.33±20.05微单位/毫升(与对照组相比P<0.05,与格列本脲相比P<0.01)。格列本脲不影响葡萄糖诱导的胰岛素释放的第一阶段(峰值为338.41±29.79微单位/毫升),但增强并延迟了第二阶段。没有药物影响胰高血糖素释放。总之,与我们测试的其他药物相比,S 21403诱导的胰岛素释放模式更快、更符合生理。

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