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在 T2DM 中使用基础胰岛素类似物或预混胰岛素类似物起始胰岛素治疗:基于治疗目标的试验的汇总分析。

Starting insulin therapy with basal insulin analog or premix insulin analog in T2DM: a pooled analysis of treat-to-target trials.

机构信息

Tulane University Health Sciences Center, New Orleans, LA 70112, USA.

出版信息

Curr Med Res Opin. 2010 Jul;26(7):1621-8. doi: 10.1185/03007995.2010.485087.

Abstract

OBJECTIVE

Although the choice of starting insulin for people with type 2 diabetes mellitus (T2DM) is often a basal or premix insulin analog, there is little evidence to base this decision on. This analysis aimed to determine if measurable clinical characteristics prior to starting insulin could predict differences in improved glycemic control between these options.

RESEARCH DESIGN AND METHODS

A thorough literature search was performed for treat-to-target studies in insulin-naïve individuals with T2DM treated with biphasic insulin aspart (BIAsp 30), a basal insulin analog (insulin glargine or insulin detemir) or NPH insulin regimens once or twice daily plus oral glucose-lowering drugs (OGLDs). Patient data were pooled and mean baseline age, diabetes duration, gender, body mass index (BMI), HbA(1c), fasting plasma glucose (FPG), average postprandial plasma glucose over three meals (PPG) and bedtime PG were investigated for prediction of improved HbA(1c), FPG or PPG. Statistical analyses employed a linear mixed model with insulin type, OGLD, time and time-squared as fixed effects and patient and trial as random effects.

RESULTS

Baseline age (p = 0.022) and bedtime PG (p = 0.036) were inter-related predictors of HbA(1c). In older individuals with higher bedtime PG, BIAsp 30 appeared to be more beneficial. In contrast, basal insulin appeared to be a better choice in younger individuals with lower bedtime PG. For FPG, BMI (p = 0.011) and post-breakfast PG (p = 0.042) were identified as predictors. Basal insulin appeared to achieve better FPG in patients with lower BMI and higher post-breakfast PG, while BIAsp 30 appeared to be better in patients with higher BMI and lower post-breakfast PG. Age (p = 0.0347) was the only baseline characteristic associated with differences in average PPG: mean PPG was similar between regimens in younger people, but BIAsp 30 achieved better PPG results in older persons. Minor hypoglycemia was reported by 56% of BIAsp 30- and 45% of basal-treated individuals. The major limitation of the study was that only Novo Nordisk trials were included in the analysis as access to individual patient data was required. As the trials were fairly heterogeneous a strict methodology was used to minimize potential confounding factors.

CONCLUSIONS

Premix analog rather than basal insulin may be an appropriate choice to target HbA(1c) values in older individuals and those with higher bedtime PG, while basal insulin may be more appropriate to target FPG in patients with lower BMI and higher post-breakfast PG.

摘要

目的

对于 2 型糖尿病(T2DM)患者,起始胰岛素治疗时通常选择基础或预混胰岛素类似物,但这种选择往往缺乏充分的依据。本分析旨在确定起始胰岛素治疗前的可测量临床特征是否可以预测这些选择方案在改善血糖控制方面的差异。

研究设计和方法

对接受双相门冬胰岛素(BIAsp 30)、基础胰岛素类似物(甘精胰岛素或地特胰岛素)或 NPH 胰岛素一日一次或两次联合口服降糖药(OGLD)治疗的新诊断 T2DM 患者的目标导向治疗研究进行了全面的文献检索。汇总患者数据,分析起始胰岛素治疗前的平均年龄、糖尿病病程、性别、体重指数(BMI)、糖化血红蛋白(HbA1c)、空腹血糖(FPG)、三餐后平均餐后血糖(PPG)和睡前血糖(PG),以预测 HbA1c、FPG 或 PPG 的改善情况。采用线性混合模型,将胰岛素类型、OGLD、时间及时间平方作为固定效应,将患者和试验作为随机效应进行统计学分析。

结果

年龄(p=0.022)和睡前 PG(p=0.036)是 HbA1c 的相关预测因素。在睡前 PG 较高的老年患者中,BIAsp 30 似乎更有益。相比之下,在睡前 PG 较低的年轻患者中,基础胰岛素可能是更好的选择。对于 FPG,BMI(p=0.011)和早餐后 PG(p=0.042)是预测因素。在 BMI 较低和早餐后 PG 较高的患者中,基础胰岛素似乎能更好地控制 FPG,而 BIAsp 30 似乎能更好地控制 BMI 较高和早餐后 PG 较低的患者的 FPG。年龄(p=0.0347)是与平均 PPG 差异相关的唯一基线特征:在年轻患者中,不同方案的平均 PPG 相似,但在老年患者中,BIAsp 30 可获得更好的 PPG 结果。56%接受 BIAsp 30 治疗和 45%接受基础胰岛素治疗的患者出现轻微低血糖。本研究的主要局限性是,由于需要获取个体患者数据,因此仅纳入了诺和诺德的试验。由于试验具有相当大的异质性,因此采用了严格的方法来最大限度地减少潜在的混杂因素。

结论

在老年患者和睡前 PG 较高的患者中,预混胰岛素类似物而非基础胰岛素可能是控制 HbA1c 值的合适选择,而在 BMI 较低和早餐后 PG 较高的患者中,基础胰岛素可能更适合控制 FPG。

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