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磺脲类药物对健康和非胰岛素依赖型糖尿病患者葡萄糖刺激的胰岛素分泌的影响:一项剂量反应研究。

Effect of sulphonylurea on glucose-stimulated insulin secretion in healthy and non-insulin dependent diabetic subjects: a dose-response study.

作者信息

Groop L C, Ratheiser K, Luzi L, Melander A, Simonson D C, Petrides A, Bonadonna R C, Widén E, DeFronzo R A

机构信息

Fourth Department of Medicine, Helsinki University Hospital, Finland.

出版信息

Acta Diabetol. 1991;28(2):162-8. doi: 10.1007/BF00579720.

DOI:10.1007/BF00579720
PMID:1777653
Abstract

The effect of a rapid-acting sulphonylurea, glipizide, on the dose-response relationship between the beta-cell response (insulin and C-peptide secretion) and the ambient plasma glucose concentration was examined in 12 healthy and 6 non-insulin-dependent diabetic subjects. The subjects participated in two sets of experiments which were performed in random order: (A) four hyperglycaemic clamp studies, during which the plasma glucose concentration was raised for 120 min by 1 (only in healthy subjects), 3, 7, and 17 mmol/l; and (B) the same four hyperglycaemic clamp studies preceded by ingestion of 5 mg glipizide. All subjects participated in a further study, in which glipizide was ingested and the plasma glucose concentration was maintained at the basal level. In control subjects in the absence of glipizide, the first-phase plasma insulin response (0-10 min) increased progressively with increasing plasma glucose concentration up to 10 mmol/l, above which it tended to plateau. Glipizide augmented the first-phase insulin response without changing the slope of the regression line relating plasma insulin to glucose concentrations. The second-phase plasma insulin response (20-120 min) increased linearly with increasing hyperglycaemia (r = 0.997). Glipizide alone increased the plasma insulin response by 180 pmol/l. A similar increase in plasma insulin response following glipizide was observed at each hyperglycaemic step, indicating that glipizide did not affect the sensitivity of the beta-cell to glucose. First-phase insulin secretion was reduced in the type 2 (non-insulin-dependent) diabetic patients, and was not influenced by glipizide.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在12名健康受试者和6名非胰岛素依赖型糖尿病患者中,研究了速效磺脲类药物格列吡嗪对β细胞反应(胰岛素和C肽分泌)与周围血浆葡萄糖浓度之间剂量反应关系的影响。受试者参与了两组随机进行的实验:(A)四项高血糖钳夹研究,在此期间,血浆葡萄糖浓度在120分钟内分别升高1(仅在健康受试者中)、3、7和17 mmol/l;(B)在摄入5 mg格列吡嗪后进行同样的四项高血糖钳夹研究。所有受试者还参与了另一项研究,即摄入格列吡嗪并将血浆葡萄糖浓度维持在基础水平。在未服用格列吡嗪的对照受试者中,第一阶段血浆胰岛素反应(0 - 10分钟)随着血浆葡萄糖浓度升高至10 mmol/l而逐渐增加,超过该浓度后趋于平稳。格列吡嗪增强了第一阶段胰岛素反应,但未改变血浆胰岛素与葡萄糖浓度之间回归线的斜率。第二阶段血浆胰岛素反应(20 - 120分钟)随着高血糖程度增加呈线性增加(r = 0.997)。单独使用格列吡嗪使血浆胰岛素反应增加了180 pmol/l。在每个高血糖阶段均观察到服用格列吡嗪后血浆胰岛素反应有类似增加,表明格列吡嗪不影响β细胞对葡萄糖的敏感性。2型(非胰岛素依赖型)糖尿病患者的第一阶段胰岛素分泌减少,且不受格列吡嗪影响。(摘要截短于250字)

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