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格列本脲和格列吡嗪对正常及非胰岛素依赖型糖尿病患者胰岛素分泌和肝葡萄糖生成的不同作用。

Different effects of glyburide and glipizide on insulin secretion and hepatic glucose production in normal and NIDDM subjects.

作者信息

Groop L, Luzi L, Melander A, Groop P H, Ratheiser K, Simonson D C, DeFronzo R A

机构信息

Yale University School of Medicine, New Haven, Connecticut.

出版信息

Diabetes. 1987 Nov;36(11):1320-8. doi: 10.2337/diab.36.11.1320.

Abstract

Glyburide (GB) and glipizide (GZ) differ in their pharmacokinetics, but it is not known whether they also differ in mode of action. To examine this question, 10 young healthy subjects and 6 non-insulin-dependent diabetic (NIDDM) patients participated in each of three studies: 1) infusion of saline for 120 min followed by a 100-min hyperglycemic (125 mg/dl) clamp; 2) 120-min primed continuous infusion of GZ followed by a 100-min hyperglycemic clamp; and 3) 120-min primed continuous infusion of GB followed by a 100-min hyperglycemic clamp. The GB and GZ infusions were continued throughout the hyperglycemic clamp. Similar plasma concentrations of GB and GZ were obtained in both groups. All studies were performed with [3-3H]glucose to allow quantification of hepatic glucose production. When administered under basal conditions of glycemia, the acute phase (0-10 min) of plasma insulin and C-peptide increase in both control and NIDDM subjects was twice as great with GZ compared with GB (P less than .01). During the hyperglycemic-clamp studies performed in normal subjects, both GB and GZ increased the first- (1.6-fold) and second- (2.2-fold) phase plasma insulin responses more than hyperglycemia alone. During the hyperglycemic clamp in NIDDM subjects, the first-phase plasma insulin response was absent, and the second-phase insulin response was markedly impaired. Neither GB nor GZ improved first-phase insulin secretion in the NIDDM patients. In both NIDDM and control subjects, the effects of hyperglycemia and sulfonylurea drugs (both GB and GZ) on the first- and second-phase plasma insulin responses were simply additive.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

格列本脲(GB)和格列吡嗪(GZ)在药代动力学方面存在差异,但它们在作用方式上是否也存在差异尚不清楚。为了研究这个问题,10名年轻健康受试者和6名非胰岛素依赖型糖尿病(NIDDM)患者参与了三项研究中的每一项:1)输注生理盐水120分钟,随后进行100分钟的高血糖(125mg/dl)钳夹;2)先进行120分钟的GZ负荷持续输注,随后进行100分钟的高血糖钳夹;3)先进行120分钟的GB负荷持续输注,随后进行100分钟的高血糖钳夹。在整个高血糖钳夹过程中持续输注GB和GZ。两组中GB和GZ的血浆浓度相似。所有研究均使用[3-3H]葡萄糖进行,以定量肝脏葡萄糖生成。在血糖基础条件下给药时,与GB相比,对照组和NIDDM受试者血浆胰岛素和C肽升高的急性期(0-10分钟),GZ的升高幅度是GB的两倍(P<0.01)。在正常受试者进行的高血糖钳夹研究中,GB和GZ均使第一相(1.6倍)和第二相(2.2倍)血浆胰岛素反应比单独高血糖时增加更多。在NIDDM受试者的高血糖钳夹过程中,第一相血浆胰岛素反应缺失,第二相胰岛素反应明显受损。GB和GZ均未改善NIDDM患者的第一相胰岛素分泌。在NIDDM和对照组受试者中,高血糖和磺脲类药物(GB和GZ)对第一相和第二相血浆胰岛素反应的影响只是简单相加。(摘要截断于250字)

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