Clinical and Experimental Endocrinology, University Hospital Leuven, Leuven, Belgium.
Atlanta Diabetes Associates, Atlanta, Georgia.
Diabetes Obes Metab. 2018 May;20(5):1148-1155. doi: 10.1111/dom.13205. Epub 2018 Feb 4.
To compare the safety and efficacy of fast-acting insulin aspart (faster aspart) with conventional insulin aspart (IAsp) in adults with type 1 diabetes (T1D).
onset 1 was a randomized, multicentre, treat-to-target, phase III, 52-week (initial 26 weeks + additional 26 weeks) trial conducted at 165 sites across 9 countries. Adults with T1D were randomly allocated to double-blind mealtime faster aspart or IAsp, each with once- or twice-daily insulin detemir. The primary endpoint, change in glycated haemoglobin (HbA1c) from baseline after the initial 26 weeks, has been reported previously. In the present paper, we report data from the full 52-week study period.
Between August 2013 and June 2015, 381 participants were assigned to double-blind faster aspart and 380 participants to IAsp. After 52 weeks, estimated mean changes from baseline in HbA1c levels were -0.08% (faster aspart) and +0.01% (IAsp); estimated treatment difference significantly favoured faster aspart (-0.10% [95% confidence interval {CI} -0.19;-0.00]; P = .0424). Changes from baseline in 1-hour postprandial plasma glucose (PPG) increment (meal test; faster aspart -1.05 mmol/L; IAsp -0.14 mmol/L) also significantly favoured faster aspart (estimated treatment difference -0.91 mmol/L [95% CI -1.40;-0.43]; -16.48 mg/dL [95% CI -25.17;-7.80]; P = .0002). There was no difference in overall severe or blood glucose-confirmed hypoglycaemic episodes or treatment-emergent adverse events between treatments.
At 52 weeks, overall glycaemic control had significantly improved with faster aspart vs IAsp, consistent with the 26-week study findings. Achieving an insulin profile closer to physiological insulin secretion with faster aspart translates into lower PPG and HbA1c levels compared with those achieved with IAsp in people with T1D.
比较速效门冬胰岛素(faster aspart)与常规门冬胰岛素(IAsp)在 1 型糖尿病(T1D)成人患者中的安全性和疗效。
ONSET 1 是一项在 9 个国家的 165 个地点进行的、随机、多中心、以目标为导向、为期 52 周(初始 26 周+额外 26 周)的 III 期临床试验。T1D 成人患者被随机分配至双盲用餐时速效门冬胰岛素或 IAsp,两者均联合每日 1 次或 2 次地特胰岛素。主要终点为初始 26 周后自基线的糖化血红蛋白(HbA1c)变化,此前已有报道。在本文中,我们报告了整个 52 周研究期间的数据。
2013 年 8 月至 2015 年 6 月,381 名患者被分配至双盲速效门冬胰岛素组,380 名患者被分配至 IAsp 组。52 周后,HbA1c 水平自基线的估计平均变化分别为-0.08%(速效门冬胰岛素)和+0.01%(IAsp);速效门冬胰岛素治疗差异显著优于 IAsp(-0.10%[95%置信区间{CI}:-0.19;-0.00];P=0.0424)。餐后 1 小时血浆葡萄糖(PPG)增量(进餐试验)自基线的变化(速效门冬胰岛素-1.05mmol/L;IAsp-0.14mmol/L)也明显有利于速效门冬胰岛素(估计治疗差异-0.91mmol/L[95%CI:-1.40;-0.43];-16.48mg/dL[95%CI:-25.17;-7.80];P=0.0002)。两种治疗方法之间总体严重低血糖或血糖确认的低血糖发作或治疗出现的不良事件无差异。
52 周时,与 IAsp 相比,速效门冬胰岛素使总体血糖控制明显改善,这与 26 周研究结果一致。与 IAsp 相比,速效门冬胰岛素使胰岛素谱更接近生理性胰岛素分泌,从而使 PPG 和 HbA1c 水平降低,这在 T1D 患者中得到证实。
