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Different effects of two dipeptidyl peptidase‐4 inhibitors and glimepiride on β ‐cell function in a newly designed two‐step hyperglycemic clamp 应用双重高糖钳夹新技术比较两种DPP‐IV抑制剂与格列美脲对胰岛 β 细胞功能的不同影响
Author(s) -
Zhang Yifei,
Chi Jie,
Wang Weiqing,
Hong Jie,
Gu Weiqiong,
Wang Bokai,
Ning Guang
Publication year - 2015
Publication title -
journal of diabetes
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.949
H-Index - 43
eISSN - 1753-0407
pISSN - 1753-0393
DOI - 10.1111/1753-0407.12175
Subject(s) - glimepiride , sitagliptin , saxagliptin , medicine , endocrinology , incretin , sitagliptin phosphate , insulin , glucagon like peptide 1 , dipeptidyl peptidase 4 , glucose clamp technique , diabetes mellitus , type 2 diabetes , metformin , insulin resistance , pancreatic hormone
Background Dipeptidyl peptidase ( DPP )‐4 inhibitors and sulfonylureas may have different effects on islet function. We designed a new two‐step hyperglycemic clamp to further compare the effects of sitagliptin, saxagliptin, and glimepiride on β‐cell function and the incretin effect. Methods The present study was a four‐way cross‐over open label randomized study. Twelve healthy male subjects were administered a single dose of sitagliptin (100 mg), saxagliptin (5 mg), glimepiride (2 mg) or blank control 2 h before undergoing a two‐step hyperglycemic clamp (Step 1: only intravenous glucose was administered; Step 2: i.v. glucose loading was combined with oral glucose consumption). Two‐phase insulin secretion, glucagon secretion, and incretin levels were measured during the clamp. Results In Step 1, with i.v. glucose only, there were no differences between the effects of the three drugs on insulin secretion, except that saxagliptin increased second‐phase insulin secretion more than glimepiride ( P = 0.007). In Step 2, oral glucose consumption led to an approximate two fold increase in insulin secretion and both gliptins significantly increased first‐phase insulin secretion compared with glimepiride ( P = 0.003 for both). Saxagliptin further increased second‐phase insulin secretion compared with glimepiride ( P = 0.005) and sitagliptin ( P < 0.001). Both gliptins significantly decreased glucagon secretion and increased active glucagon‐like peptide‐1 ( GLP ‐1) compared with glimepiride, especially in Step 2. Conclusions The two‐step hyperglycemic clamp appears to be a precise method to assess β‐cell function by taking the effect of incretins into consideration. The oral glucose consumption adds to the i.v. glucose infusion, amplifying the differences in the effects of DPP ‐4 inhibitors and glimepiride on insulin secretion.

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