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首页> 外文期刊>Diabetes care >Early pharmacokinetic and pharmacodynamic effects of mixing lispro with glargine insulin: results of glucose clamp studies in youth with type 1 diabetes.
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Early pharmacokinetic and pharmacodynamic effects of mixing lispro with glargine insulin: results of glucose clamp studies in youth with type 1 diabetes.

机译:赖脯胰岛素与甘精胰岛素混合的早期药代动力学和药效学作用:青年1型糖尿病患者的葡萄糖钳夹研究结果。

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OBJECTIVE Clinicians who treat children with type 1 diabetes often try to minimize the number of daily injections to reduce treatment burden and improve compliance. Despite the manufacturer's cautions against mixing glargine with rapid-acting insulin analogs, clinical studies have failed to demonstrate deleterious effects of mixing on glucose excursions or A1C levels. However, no formal glucose clamp studies have been performed to determine whether mixing with glargine has an adverse effect on the early pharmacodynamic action of rapid-acting insulin in humans. RESEARCH DESIGN AND METHODS To examine this question, euglycemic glucose clamps were performed twice, in random order, in 11 youth with type 1 diabetes (age 15.1 +/- 3 years, A1C 7.6 +/- 0.6%) with 0.2 units/kg lispro and 0.4 units/kg glargine, given either as separate or as a single mixed injection. RESULTS Mixing the two insulins shifted the time action curve to the right, with significantly lower glucose infusion rate (GIR) values after the mixed injections between 60 and 190 min and significantly higher values between 270 and 300 min, lowered the GIR(max) (separate 7.1 +/- 1 vs. mix 3.9 +/- 1, P = 0.03), and markedly delayed the time to reach GIR(max) (separate 116 +/- 8 min vs. mix 209 +/- 15 min, P = 0.004). The GIR area under the curve was significantly lower after the mixed injections. Mixing had similar effects on plasma insulin pharmacokinetics. CONCLUSIONS These data demonstrate that mixing lispro with glargine markedly flattens the early pharmacodynamic peak of lispro and causes a shift to the right in the GIR curve changes that might lead to difficulties in controlling meal-related glucose excursions.
机译:目的治疗1型糖尿病儿童的临床医生经常尝试减少每日注射次数,以减轻治疗负担并改善依从性。尽管制造商警告不要将甘精胰岛素与速效胰岛素类似物混合,但临床研究未能证明混合对葡萄糖偏移或A1C水平有有害影响。然而,尚未进行正式的葡萄糖钳夹研究来确定与甘精胰岛素混合是否对速效胰岛素在人体中的早期药效作用产生不利影响。研究设计与方法为了研究这个问题,对11名1型糖尿病青年(年龄15.1 +/- 3岁,A1C 7.6 +/- 0.6%)以0.2单位/千克的赖脯胰岛素进行了随机血糖检查和0.4单位/公斤的甘精胰岛素,可以单独注射或一次混合注射。结果两种胰岛素的混合使时间作用曲线向右移动,混合注射60至190分钟后葡萄糖输注速率(GIR)值显着降低,而270至300分钟之间显着较高的值降低了GIR(max)(分别为7.1 +/- 1与混合3.9 +/- 1,P = 0.03),并显着延迟了达到GIR(max)的时间(分别为116 +/- 8分钟与混合209 +/- 15分钟,P = 0.004)。混合进样后,曲线下的GIR面积显着降低。混合对血浆胰岛素药代动力学具有相似的影响。结论这些数据表明,赖脯胰岛素与甘精氨酸混合显着使赖脯胰岛素的早期药效学峰变平,并导致GIR曲线变化向右移动,这可能导致难以控制与餐有关的葡萄糖偏移。

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