PHARMO Institute, Utrecht, The Netherlands.
Adv Ther. 2010 Apr;27(4):211-22. doi: 10.1007/s12325-010-0020-y. Epub 2010 May 4.
The objective was to compare glycemic control, insulin utilization, and body weight in patients with type 2 diabetes (T2D) initiated on insulin detemir (IDet) or insulin glargine (IGlar) in a real-life setting in the Netherlands.
Insulin-naïve patients with T2D, starting treatment with IDet or IGlar between January 1, 2004 and June 30, 2008, were selected from the PHARMO data network. Glycemic control (hemoglobin A1c [HbA1c]), target rates (HbA1c <7%), daily insulin dose, and weight gain were analyzed comparing IDet and IGlar for patients with available HbA1c levels both at baseline and at 1-year follow-up. Analysis of all eligible patients (AEP) and a subgroup of patients without treatment changes (WOTC) in the follow-up period were adjusted for patient characteristics, propensity scores, and baseline HbA1c.
A total of 127 IDet users and 292 IGlar users were included in the WOTC analyses. The mean HbA1c dropped from 8.4%-8.6% at baseline to 7.4% after 1 year. Patients at HbA1c goal increased from 9% at baseline to 32% for IDet and 11% to 35% for IGlar, which was not significantly different (OR 0.75, 95% CI 0.46, 1.24). Weight gain (n=90) was less among IDet users (+0.4 kg) than among IGlar users (+1.1 kg), albeit not significant. The AEP analysis (252 IDet + 468 IGlar users) showed similar results with 33%-36% at goal (OR 0.81, 95% CI 0.57, 1.16), and median daily insulin doses of 25 IU/day (P=0.70).
There was no significant difference between users of IDet and IGlar with respect to glycemic control and insulin dose in a real-life setting. The low proportion of patients on target at baseline may indicate that insulin therapy is initiated too late. Moreover, the observation that one-third of the patients reached HbA1c target at follow-up may indicate that basal insulin analogs are not titrated intensively enough.
本研究旨在比较在荷兰的真实环境下,新诊断为 2 型糖尿病(T2D)的患者起始胰岛素地特胰岛素(IDet)或甘精胰岛素(IGlar)治疗后的血糖控制、胰岛素利用和体重变化。
从 PHARMO 数据网络中选择 2004 年 1 月 1 日至 2008 年 6 月 30 日期间起始胰岛素治疗且为胰岛素初治的 T2D 患者,比较基线和 1 年随访时均有糖化血红蛋白(HbA1c)值的患者中 IDet 和 IGlar 治疗的血糖控制(HbA1c)、达标率(HbA1c<7%)、每日胰岛素剂量和体重增加情况。对所有符合条件的患者(AEP)和随访期间无治疗变更的患者(WOTC)进行分析,调整患者特征、倾向评分和基线 HbA1c。
WOTC 分析中纳入了 127 例 IDet 使用者和 292 例 IGlar 使用者。HbA1c 从基线时的 8.4%-8.6%降至 1 年后的 7.4%。HbA1c 达标患者比例从基线时的 9%增至 IDet 组的 32%和 IGlar 组的 35%,但无显著差异(OR 0.75,95%CI 0.46,1.24)。IDet 使用者的体重增加(n=90)较 IGlar 使用者(+1.1kg)少(+0.4kg),但无统计学意义。AEP 分析(252 例 IDet+468 例 IGlar 使用者)显示出相似的结果,目标范围内的患者比例为 33%-36%(OR 0.81,95%CI 0.57,1.16),且每日胰岛素剂量中位数为 25IU/天(P=0.70)。
在真实环境中,IDet 和 IGlar 的使用者在血糖控制和胰岛素剂量方面无显著差异。基线时达标患者比例较低可能表明胰岛素治疗开始得太晚。此外,三分之一的患者在随访时达到 HbA1c 目标,这可能表明基础胰岛素类似物的滴定不够积极。
