National Research Institute, Los Angeles California, United States.
Diabetes Center Bochum-Hattingen, St Josef Hospital, Ruhr-University Bochum, Bochum, Germany.
Diabetes Obes Metab. 2020 Jun;22(6):938-946. doi: 10.1111/dom.13979. Epub 2020 Feb 11.
To assess the efficacy and tolerability of tirzepatide treatment using three different dose-escalation regimens in patients with type 2 diabetes.
In this double-blind, placebo-controlled study, patients were randomized (1:1:1:1) to receive either once-weekly subcutaneous tirzepatide or placebo. The tirzepatide dose groups and dose-escalation regimens were: 12 mg (4 mg weeks 0-3; 8 mg weeks 4-7; 12 mg weeks 8-11), 15 mg-1 (2.5 mg weeks 0-1; 5 mg weeks 2-3; 10 mg weeks 4-7; 15 mg weeks 8-11) and 15 mg-2 (2.5 mg weeks 0-3; 7.5 mg weeks 4-7; 15 mg weeks 8-11). The primary objective was to compare tirzepatide with placebo in HbA1c change from baseline at 12 weeks.
Overall, 111 patients were randomized: placebo, 26; tirzepatide 12 mg, 29; tirzepatide 15 mg-1, 28; tirzepatide 15 mg-2, 28. The mean age was 57.4 years, HbA1c 8.4% and body mass index 31.9 kg/m . At week 12, absolute HbA1c change from baseline (SE) was greater in the tirzepatide treatment groups compared with placebo (placebo, +0.2% [0.21]; 12 mg, -1.7% [0.19]; 15 mg-1, -2.0% [0.20]; 15 mg-2, -1.8% [0.19]). The incidence of nausea was: placebo, 7.7%; 12 mg group, 24.1%; 15 mg-1 group, 39.3%; 15 mg-2 group, 35.7%. Three patients discontinued the treatment because of adverse events, one from each of the placebo, 12 mg and 15 mg-1 groups.
Tirzepatide treatment for 12 weeks resulted in clinically significant reductions in HbA1c. This suggests that lower starting doses and smaller dose increments are associated with a more favourable side effect profile.
评估三种不同剂量递增方案下替西帕肽治疗 2 型糖尿病患者的疗效和耐受性。
在这项双盲、安慰剂对照研究中,患者被随机(1:1:1:1)接受每周一次皮下注射替西帕肽或安慰剂。替西帕肽剂量组和剂量递增方案为:12mg(4mg 周 0-3;8mg 周 4-7;12mg 周 8-11)、15mg-1(2.5mg 周 0-1;5mg 周 2-3;10mg 周 4-7;15mg 周 8-11)和 15mg-2(2.5mg 周 0-3;7.5mg 周 4-7;15mg 周 8-11)。主要目的是比较替西帕肽与安慰剂在 12 周时 HbA1c 自基线的变化。
共有 111 名患者被随机分组:安慰剂组 26 例,替西帕肽 12mg 组 29 例,替西帕肽 15mg-1 组 28 例,替西帕肽 15mg-2 组 28 例。患者平均年龄为 57.4 岁,HbA1c 为 8.4%,体重指数为 31.9kg/m 。在第 12 周时,与安慰剂相比,替西帕肽治疗组的 HbA1c 自基线的绝对变化更大(安慰剂:+0.2%[0.21];12mg:-1.7%[0.19];15mg-1:-2.0%[0.20];15mg-2:-1.8%[0.19])。恶心的发生率分别为:安慰剂组 7.7%;12mg 组 24.1%;15mg-1 组 39.3%;15mg-2 组 35.7%。有 3 名患者因不良事件停止治疗,分别来自安慰剂组、12mg 组和 15mg-1 组。
替西帕肽治疗 12 周可显著降低 HbA1c。这表明较低的起始剂量和较小的剂量递增与更有利的不良反应谱相关。
