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An analysis of early insulin glargine added to metformin with or without sulfonylurea: impact on glycaemic control and hypoglycaemia

机译:含或不含磺酰脲的二甲双胍中加入早期甘精胰岛素的分析:对血糖控制和低血糖的影响

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摘要

>Aim: To evaluate the benefits of initiating insulin at an earlier versus later treatment stage, and regimens with/without sulfonylurea (SU).>Methods: Pooled analysis of 11 prospective randomized clinical trials, including 2171 adults with uncontrolled type 2 diabetes initiating insulin glargine following a specific titration algorithm. Clinical outcomes were glycated haemoglobin A1c (HbA1c) reduction, per cent achieving HbA1c ≤ 7.0%, weight gain and hypoglycaemic events. Statistical analysis compared outcomes 24 weeks after basal insulin initiation in patients previously uncontrolled on 0/1 oral antidiabetic drug (OAD) versus 2 OADs, and in patients taking metformin (MET) or SU alone or in combination at baseline. A meta-analysis was also conducted.>Results: For the pooled analysis, patients on 0/1 OAD and those on MET monotherapy at baseline had the largest 24-week reductions in HbA1c following the addition of insulin glargine (∼0.44 U/kg). Of patients failing MET/SU monotherapy and MET + SU in combination, 68.1, 50.4 and 56.4% achieved HbA1c ≤ 7.0%, respectively (p = 0.0006). Weight gain was lowest when basal insulin was added to MET. Patients on 0/1 OAD at baseline had significantly less symptomatic hypoglycaemia when basal insulin was added than those on 2 OADs (p = 0.0007). Despite higher insulin doses, those taking MET alone had less hypoglycaemia than those taking SU or MET + SU. Results were confirmed in the meta-analysis.>Conclusion: Adding insulin glargine to MET monotherapy early in treatment may provide efficacy/safety benefits over regimens including SU. This may reflect treatment earlier in the disease and supports the inclusion of insulin as a second step in the American Diabetes Association/European Association for the Study of Diabetes treatment algorithm.
机译:>目标::评估在早期和晚期治疗阶段以及使用/不使用磺酰脲(SU)方案时开始胰岛素的益处。>方法:对11项前瞻性随机临床研究进行汇总分析临床试验,包括2171名通过特定滴定算法启动甘精胰岛素的不受控制的2型糖尿病成人。临床结果是糖化血红蛋白A1c(HbA1c)减少,HbA1c≤7.0%的百分比,体重增加和降血糖事件。统计分析比较了先前未使用0/1口服抗糖尿病药(OAD)与2种OAD进行对照的基础胰岛素起始后24周的结果,以及在基线时单独或联合服用二甲双胍(MET)或SU的患者。 >结果:对于汇总分析,添加甘精胰岛素后,0/1 OAD患者和基线行MET单药治疗的患者HbA1c降低最大,为24周(〜0.44 U / kg)。在MET / SU单药治疗和MET + SU联合治疗失败的患者中,分别达到68.1%,50.4%和56.4%的HbA1c≤7.0%(p = 0.0006)。当基础胰岛素添加到MET中时,体重增加最低。添加基础胰岛素时,基线时以0/1 OAD进行治疗的患者的症状性低血糖症明显少于2次OAD(p = 0.0007)。尽管胰岛素剂量较高,但仅服用MET的人的低血糖症要比服用SU或MET + SU的人低。荟萃分析证实了结果。>结论:在治疗早期,将甘精胰岛素加入MET单药治疗可能比包括SU在内的治疗方案具有疗效/安全性。这可能反映了疾病的早期治疗,并支持将胰岛素纳入美国糖尿病协会/欧洲糖尿病研究算法研究协会的第二步。

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