首页> 美国卫生研究院文献>Springer Open Choice >Starting bedtime glargine versus NPH insulin in poorly controlled type 2 diabetic patients with various hyperglycemia types (fasting type or postprandial type)
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Starting bedtime glargine versus NPH insulin in poorly controlled type 2 diabetic patients with various hyperglycemia types (fasting type or postprandial type)

机译:在患有各种高血糖类型(禁食型或餐后型)的血糖控制不佳的2型糖尿病患者中开始睡前服用甘精胰岛素与NPH胰岛素

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摘要

Our aim was to compare the effects of an intermediate acting human insulin (NPH) and a long-acting insulin analog, insulin glargine, in insulin naïve type 2 diabetes patients, stratified by the type of hyperglycemia (fasting or postprandial type). Based on different action profiles, we hypothesized that patients having different hyperglycemia types would react differently when treated with these insulins. This is a post hoc analysis of the Lanmet study data. The Lanmet study was a randomized, 36-week controlled insulin initiation study in type 2 diabetes patients. 109 subjects with baseline HbA1c >8.0 % (64 mmol/mol) completed the study. The patients were divided into two groups according to fasting glucose (mmol/l)/HbA1c (%) ratio. Patients with a ratio ≥1.3 were defined as having fasting type and those with a ratio <1.3 as having postprandial type hyperglycemia. The main outcome measures were change in HbA1c and body weight, and final insulin dose. Independently of insulin type, compared to patients with postprandial type hyperglycemia, those with fasting type hyperglycemia had 2.1 kg/m2 greater initial BMI (p = 0.044), gained 2.0 kg more weight (p = 0.020, adjusted for baseline BMI p = 0.035), and had 36 % greater final insulin dose/kg (p = 0.001). With respect to hyperglycemia type, there was no difference between NPH and glargine in their effects on HbA1c. When starting bedtime insulin in type 2 diabetes patients, those with fasting type hyperglycemia are prone to greater weight gain. Hyperglycemia type does not help in identifying patients who would benefit specially from either NPH insulin or insulin glargine.
机译:我们的目的是比较中效人胰岛素(NPH)和长效胰岛素类似物甘精胰岛素对2型糖尿病初治糖尿病患者的影响,并按高血糖类型(空腹或餐后类型)进行分层。基于不同的作用模式,我们假设具有不同高血糖类型的患者在用这些胰岛素治疗时会产生不同的反应。这是Lanmet研究数据的事后分析。 Lanmet研究是针对2型糖尿病患者的一项为期36周的随机对照胰岛素起始研究。 109名基线HbA1c> 8.0%(64 mmol / mol)的受试者完成了研究。根据空腹血糖(mmol / l)/ HbA1c(%)的比例将患者分为两组。比率≥1.3的患者定义为空腹型,比率<1.3的患者定义为餐后高血糖。主要结局指标是HbA1c和体重的变化以及最终胰岛素剂量。与餐后高血糖患者相比,与餐后高血糖患者相比,空腹型高血糖患者的初始BMI值高2.1 kg / m 2 (p = 0.044),体重增加2.0kg(p = 0.020,调整后的基线BMI p = 0.035),并且最终胰岛素剂量/ kg增加了36%(p = 0.001)。就高血糖类型而言,NPH和甘精氨酸对HbA1c的影响没有差异。在2型糖尿病患者中开始就寝胰岛素时,那些具有禁食型高血糖症的患者倾向于增加体重。高血糖类型无助于识别将特别受益于NPH胰岛素或甘精胰岛素的患者。

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