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首页> 外文期刊>Journal of diabetes and its complications >Reduced risk of hypoglycemia with once-daily glargine versus twice-daily NPH and number needed to harm with NPH to demonstrate the risk of one additional hypoglycemic event in type 2 diabetes: Evidence from a long-term controlled trial
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Reduced risk of hypoglycemia with once-daily glargine versus twice-daily NPH and number needed to harm with NPH to demonstrate the risk of one additional hypoglycemic event in type 2 diabetes: Evidence from a long-term controlled trial

机译:每日一次甘精胰岛素与每天两次NPH相比降低了低血糖的风险,以及需要NPN损害的数量以证明2型糖尿病又发生另一次降血糖事件的风险:一项长期对照试验的证据

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摘要

Aims This analysis evaluated HbA1c-adjusted hypoglycemia risk with glargine versus neutral protamine Hagedorn (NPH) over a 5-year study in patients with Type 2 diabetes mellitus (T2DM). Clinical significance was assessed using number needed to harm (NNH) to demonstrate the risk of one additional patient experiencing at least one hypoglycemic event. Methods Individual patient-level data for symptomatic documented hypoglycemia and HbA1c values from a 5-year randomized study comparing once-daily glargine (n = 513) with twice-daily NPH (n = 504) were analyzed. Symptomatic hypoglycemia was categorized according to concurrent self-monitoring blood glucose levels and need for assistance. Hypoglycemic events per patient-year as a function of HbA1c were fitted by negative binomial regression using treatment and HbA1c at endpoint as independent variables. An estimate of NNH was derived from logistic regression models. Results The cumulative number of symptomatic hypoglycemia events was consistently lower with glargine compared with NPH over 5 years. Compared with twice-daily NPH, once-daily glargine treatment resulted in significantly lower adjusted odds ratios (OR) for all daytime hypoglycemia (OR 0.74; p = 0.030) and any severe event (OR 0.64; p = 0.035), representing a 26% and 36% reduction in the odds of daytime and severe hypoglycemia, respectively. Our model predicts that, if 25 patients were treated with NPH instead of glargine, then one additional patient would experience at least one severe hypoglycemic event. Conclusions This analysis of long-term insulin treatment confirms findings from short-term studies and demonstrates that glargine provides sustained, clinically meaningful reductions in risk of hypoglycemia compared with NPH in patients with T2DM.
机译:目的这项分析在为期2年的2型糖尿病(T2DM)患者中进行了为期5年的研究,评估了甘精胰岛素与中性鱼精蛋白Hagedorn(NPH)联合HbA1c调整的低血糖风险。使用伤害需要数量(NNH)评估临床意义,以证明另一名患者发生至少一项降血糖事件的风险。方法分析了一项为期5年的随机研究的有症状的低血糖和HbA1c值的个体患者水平数据,该研究将每日一次甘精胰岛素(n = 513)与每天两次NPH(n = 504)进行了比较。有症状的低血糖症是根据同时进行的自我监测血糖水平和需要帮助进行分类的。使用治疗和终点HbA1c作为独立变量,通过负二项式回归拟合每患者每年的降血糖事件,作为HbA1c的函数。 NNH的估计是从逻辑回归模型得出的。结果5年来,甘精胰岛素的症状性低血糖事件的累积发生率一直低于NPH。与每天两次NPH相比,每天一次甘精胰岛素治疗导致全天低血糖(OR 0.74; p = 0.030)和任何严重事件(OR 0.64; p = 0.035)的调整比值比(OR)显着降低,代表26白天和严重低血糖的几率分别降低了%和36%。我们的模型预测,如果25例患者接受NPH代替甘精胰岛素治疗,那么另一名患者将经历至少一次严重的降血糖事件。结论这项对长期胰岛素治疗的分析证实了短期研究的结果,并证明与2型糖尿病患者相比,甘精胰岛素与NPH相比具有持续,临床意义的低血糖风险降低。

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