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通过持续葡萄糖监测系统评估甘精胰岛素作为基础胰岛素替代物的优越性。

Evaluation of the superiority of insulin glargine as basal insulin replacement by continuous glucose monitoring system.

作者信息

Wang Xian Ling, Lu Ju Ming, Pan Chang Yu, Mu Yi Ming, Dou Jing Tao, Ba Jian Ming, Wang Xuemin

机构信息

Department of Endocrinology, Chinese PLA General Hospital, Fu Xing Road 28, Beijing 100853, China.

出版信息

Diabetes Res Clin Pract. 2007 Apr;76(1):30-6. doi: 10.1016/j.diabres.2006.08.005. Epub 2006 Sep 15.

Abstract

To evaluate the superiority of insulin glargine as basal insulin replacement by continuous glucose monitoring system (CGMS). Twenty-four patients with type 2 diabetes mellitus (T2DM) whose blood glucose was not well controlled with sulphanylureas were enrolled. At first, they were treated with extended-release glipizide (glucotrol XL) 5mg/d before breakfast for 2 weeks, then randomized to combination treatment with glargine (16 patients) or NPH (8 patients) and treated for 12 weeks. CGMS were carried in the second week after treatment with glucotrol XL, and in the 12th week after combination treatment. The data of CGMS showed: (1) When FPG were well controlled in both groups (glargine group versus NPH group: 6.0+/-1.0 mmol/L versus 5.8+/-1.3 mmol/L), the blood glucose level at 3:00 a.m. (5.1+/-0.9 mmol/L versus 4.2+/-0.8 mmol/L) were higher (P<0.05), TPG< or =3.0 mmol/L at night were lower (2.56+/-1.79 versus 5.88+/-1.96), and the rate of nocturnal hypoglycemia (1/16 versus 4/8) were less (P=0.028) in glargine group than those in NPH group. (2) CGMS showed that the daily blood glucose profile excursion were more smoother in glargine group than those in NPH group. In conclusion, it was confirmed with CGMS that compared with traditionally basal insulin replacement with NPH, the combination treatment with glargine injection at bedtime may be predominant for stabilizing the daily blood glucose profile excursion and decreasing the nocturnal hypoglycemia events incidence. So glargine may be a more ideal basal insulin replacement than NPH.

摘要

通过连续血糖监测系统(CGMS)评估甘精胰岛素作为基础胰岛素替代治疗的优越性。纳入24例使用磺脲类药物血糖控制不佳的2型糖尿病(T2DM)患者。起初,他们早餐前服用5mg/d的缓释格列吡嗪(优降糖XL)治疗2周,然后随机分为甘精胰岛素联合治疗组(16例)和中性鱼精蛋白锌胰岛素(NPH)联合治疗组(8例),治疗12周。在使用优降糖XL治疗后的第2周以及联合治疗后的第12周进行CGMS监测。CGMS数据显示:(1)两组空腹血糖(FPG)均得到良好控制时(甘精胰岛素组与NPH组:6.0±1.0 mmol/L对5.8±1.3 mmol/L),凌晨3点的血糖水平(5.1±0.9 mmol/L对4.2±0.8 mmol/L)甘精胰岛素组更高(P<0.05),夜间血糖≤3.0 mmol/L的情况更少(2.56±1.79对5.88±1.96),且甘精胰岛素组夜间低血糖发生率(1/16对4/8)低于NPH组(P=0.028)。(2)CGMS显示甘精胰岛素组的每日血糖波动曲线比NPH组更平滑。总之,CGMS证实与传统的NPH基础胰岛素替代治疗相比,睡前注射甘精胰岛素联合治疗在稳定每日血糖波动曲线及降低夜间低血糖事件发生率方面可能更具优势。因此,甘精胰岛素可能是比NPH更理想的基础胰岛素替代药物。

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