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首页> 外文期刊>Medicine. >Impact of patient and treatment characteristics on glycemic control and hypoglycemia in patients with type 2 diabetes initiated to insulin glargine or NPH: A post hoc, pooled, patient-level analysis of 6 randomized controlled trials
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Impact of patient and treatment characteristics on glycemic control and hypoglycemia in patients with type 2 diabetes initiated to insulin glargine or NPH: A post hoc, pooled, patient-level analysis of 6 randomized controlled trials

机译:患者和治疗特点对甘精胰岛素或NPH引发的2型糖尿病患者血糖控制和低血糖的影响:一项针对6项随机对照试验的事后,汇总,患者水平分析

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Background: The goal of this post hoc analysis was to determine key patient and treatment-related factors impacting glycosylated hemoglobin (A1C) and hypoglycemia in patients with uncontrolled type 2 diabetes who were initiated to basal insulin (neutral protamine Hagedorn [NPH] or glargine). Methods: Using individual patient-level data pooled from 6 treat-to-target trials, 2600 patients with type 2 diabetes on oral antidiabetic agents initiated to insulin glargine or NPH and treated for 24 to 36 weeks were analyzed. Results: Both treatments led to significant reduction in A1C levels compared with baseline, with no differences between treatment groups (mean ± standard deviation; glargine: ?1.32 ± 1.2% vs NPH: ?1.26 ± 1.2%; P = 0.15), with greater reduction in the BMI ≥30 kg/m2 group than in the BMI 2 group. Glargine reduced A1C significantly more than NPH in the BMI 2 group (?1.30 ± 1.18% vs ?1.14 ± 1.22, respectively; P = 0.008), but not in the BMI ≥ 30 kg/m2 group (?1.37 ± 1.19 vs ?1.48 ± 1.22, respectively; P = 0.18). Similar proportions of patients achieved A1C target of 2 group. Conclusions: Initiation of basal insulin is highly effective in lowering A1C after oral antidiabetic agent failure. Glargine decreases A1C more than NPH in nonobese patients, and reduces the risk for severe and severe nocturnal hypoglycemia versus NPH both in obese and nonobese patients, but more so in nonobese patients. Thus, it is the nonobese patients who may benefit more from initiation of basal insulin as glargine than NPH.
机译:背景:这项事后分析的目的是确定影响基础胰岛素(中性鱼精蛋白Hagedorn [NPH]或甘精胰岛素)的非控制性2型糖尿病患者中影响糖基化血红蛋白(A1C)和低血糖的关键患者和与治疗相关的因素。方法:使用从6项针对治疗的试验中收集的个体患者水平数据,分析2600例接受口服甘精胰岛素或NPH口服抗糖尿病药并治疗24至36周的2型糖尿病患者。结果:与基线相比,两种治疗均导致A1C水平显着降低,各治疗组之间无差异(平均值±标准差;甘精氨酸:?1.32±1.2%,NPH:?1.26±1.2%; P = 0.15),且更大与BMI 2 组相比,BMI≥30 kg / m 2 组的减少。甘精胰岛素在BMI 2 组中对A1C的抑制作用明显大于NPH(分别为1.30±1.18%和1.14±1.22; P = 0.008),但在BMI≥30 kg / m的情况下没有降低=“ http://webservices.ovid.com/mrws/1.0”> 2 组(分别为1.37±1.19和1.48±1.22; P = 0.18)。达到2 组A1C目标的患者比例相似。结论:口服抗糖尿病药失败后,基础胰岛素的启动可有效降低A1C。非肥胖患者中,甘精胰岛素比NPH降低的A1C更大,并且无论肥胖还是非肥胖患者,与NPH相比,降低严重和严重的夜间低血糖的风险更大,而非肥胖患者则更是如此。因此,非肥胖患者从基础胰岛素(甘精胰岛素)的治疗中受益的可能性要大于NPH。

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