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格列齐特对II型糖尿病患者胃抑制性多肽(GIP)无影响。

No effect of gliclazide on gastric inhibitory polypeptide (GIP) in type II diabetes.

作者信息

Scott R S, Donnelly T

出版信息

Diabetes Res Clin Pract. 1987 May-Jun;3(3):175-8. doi: 10.1016/s0168-8227(87)80024-4.

Abstract

Seven subjects with non-insulin-dependent diabetes mellitus were studied prior to and after 1 month of treatment with gliclazide, 80 mg twice daily. Individuals attended for a standard breakfast test meal (10 kcal/kg) on three occasions--prior to therapy, first day of therapy, and 30th day of therapy. Blood samples were collected between 0 and 240 min post-prandially and assayed for glucose, insulin, C-peptide, glucagon, pancreatic polypeptide, gastric inhibitory polypeptide (GIP), and gastrin. Following gliclazide, fasting and post-prandial glucose levels were significantly improved. An increase in post-prandial insulin and C-peptide levels was noted on the first treatment day and values remained elevated for the study period. GIP and other measured peptide hormones were unchanged. These data suggest that gliclazide asserts its hypoglycaemic effects by promoting insulin release, and has no detectable effect on other enteropancreatic hormones.

摘要

对7名非胰岛素依赖型糖尿病患者在接受每日两次、每次80毫克格列齐特治疗1个月前后进行了研究。受试者在三个时间点参加标准早餐测试餐(10千卡/千克)——治疗前、治疗第一天和治疗第30天。在餐后0至240分钟之间采集血样,检测血糖、胰岛素、C肽、胰高血糖素、胰多肽、胃抑肽(GIP)和胃泌素。服用格列齐特后,空腹和餐后血糖水平显著改善。在治疗第一天观察到餐后胰岛素和C肽水平升高,且在研究期间这些值一直保持升高。GIP和其他检测的肽类激素未发生变化。这些数据表明,格列齐特通过促进胰岛素释放发挥其降血糖作用,并且对其他胃肠胰激素没有可检测到的影响。

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