Abbink Evertine J, van der Wal Pieter S, Sweep C G J Fred, Smits Paul, Tack Cees J
Department of Internal Medicine, University Medical Centre, Nijmegen, The Netherlands.
Diabetes Metab Res Rev. 2004 Nov-Dec;20(6):466-71. doi: 10.1002/dmrr.474.
The more rapid onset of action and the shorter half-life of repaglinide may reduce the post-load glucose excursion and limit sustained insulin secretion compared to sulphonylurea (SU) derivatives.
We studied 12 patients with type 2 diabetes (age 62 +/- 2 years, BMI 28.3 +/- 1.3 kg m(-2), HbA1c 6.7 +/- 0.2%) on SU monotherapy at submaximal dose. Patients were treated for 3 weeks with repaglinide or glibenclamide in a randomized, crossover trial. At the end of each treatment period, patients underwent a 60-min hyperglycaemic clamp (glucose 12 mmol L(-1)) followed by 4-h observation (60-300 min) with frequent blood sampling for determination of glucose, insulin, proinsulin and C-peptide levels. Before the clamp (5 min for repaglinide, 30 min for glibenclamide), patients ingested their usual morning drug dose.
After the end of the hyperglycaemic clamp, mean plasma glucose fell to a level of 5 mmol L(-1) after approximately 150 min with repaglinide, and after approximately 190 min with glibenclamide. While initially quite similar, in the period from 240 to 300 min, insulin, proinsulin and C-peptide levels were lower during repaglinide treatment (insulin 133 +/- 20 vs 153 +/- 25 pmol L(-1) (P < 0.05), proinsulin 14 +/- 3 vs 19 +/- 4 pmol L(-1) (P = 0.06) and C-peptide 0.81 +/- 0.19 vs 1.14 +/- 0.18 nmol L(-1) (P = 0.05) for repaglinide vs glibenclamide, respectively).
Following glucose stimulation, plasma glucose levels, and insulin concentration decrease more rapidly after repaglinide treatment than after glibenclamide. Proinsulin and C-peptide secretion tended to fall more rapidly as well. These findings are consistent with a more rapid onset and shorter duration of beta-cell stimulation associated with repaglinide.
与磺脲类(SU)衍生物相比,瑞格列奈起效更快、半衰期更短,可能会减少负荷后血糖波动并限制胰岛素的持续分泌。
我们研究了12例接受次最大剂量SU单药治疗的2型糖尿病患者(年龄62±2岁,体重指数28.3±1.3 kg/m²,糖化血红蛋白6.7±0.2%)。在一项随机交叉试验中,患者分别接受瑞格列奈或格列本脲治疗3周。在每个治疗期结束时,患者接受60分钟的高血糖钳夹试验(血糖12 mmol/L),随后进行4小时观察(60 - 300分钟),期间频繁采血以测定血糖、胰岛素、胰岛素原和C肽水平。在钳夹试验前(瑞格列奈为5分钟,格列本脲为30分钟),患者服用其常规的早晨药物剂量。
高血糖钳夹试验结束后,瑞格列奈治疗组患者的平均血浆葡萄糖在约150分钟后降至5 mmol/L水平,格列本脲治疗组则在约190分钟后降至该水平。虽然最初两者相当相似,但在240至300分钟期间,瑞格列奈治疗期间胰岛素、胰岛素原和C肽水平较低(瑞格列奈组与格列本脲组相比,胰岛素分别为133±20对153±25 pmol/L(P<0.05),胰岛素原为14±3对19±4 pmol/L(P = 0.06),C肽为0.81±0.19对1.14±0.18 nmol/L(P = 0.05))。
葡萄糖刺激后,瑞格列奈治疗后的血浆葡萄糖水平和胰岛素浓度下降速度比格列本脲更快。胰岛素原和C肽分泌也倾向于下降得更快。这些发现与瑞格列奈相关的β细胞刺激起效更快、持续时间更短一致。