用SMBG测量轻度2型糖尿病患者格列美脲滴定的有效性

A. Kanazawa, Tomoaki Shimizu, C. Ebato, Yuko Sakurai, N. Kumashiro, Shinya Miwa, T. Hirose, Yasushi Tanaka, R. Kawamori, H. Watada
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引用次数: 2

摘要

格列美脲是一种有效的磺脲类药物,广泛用于2型糖尿病患者,然而,格列美脲在糖尿病控制良好(HbA1c水平:6.5-7.9%)患者中的安全性和有效性尚未得到研究。因此,我们研究了采用自我监测血糖(SMBG)的格列美脲滴定法在相当控制的糖尿病患者中实现严格血糖控制的安全性和有效性。将饮食控制或α -葡萄糖苷酶抑制剂或二甲双胍治疗的日本2型糖尿病患者随机分为使用SMBG滴定格列美脲的SMBG组和不使用SMBG的常规治疗组(对照组)。格列美脲起始剂量为0.5 mg/天,两组患者在6个月的时间内评估血糖、胰岛素、糖化血红蛋白和糖蛋白水平。SMBG组根据早餐和晚餐前的SMBG水平滴定格列美脲的剂量。6个月时,SMBG组格列美脲的平均剂量倾向于高于对照组(1.0±0.8 mg/天vs 0.6±0.3mg/天),但不显著。在格列美脲治疗6个月后,两组患者的HbA1c水平显著低于基线水平(SMBG: 7.2±0.5 vs 6.5±0.6%,n=23, P<0.01,对照组:7.3±0.4 vs 6.5±0.7%,n=24, P<0.01),尽管两组患者在6个月时的HbA1c水平相似。50名受试者中仅记录了3次低血糖发作。在本研究中,我们没有发现格列美脲滴定方案的疗效。然而,格列美脲显著改善血糖控制良好的糖尿病患者无严重低血糖。
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Measuring Effectiveness of Glimepiride Titration Using SMBG in Patients with Mild Type 2 Diabetes
Glimepiride is a potent sulfonylurea agent and is widely used for type 2 diabetic patients, however, the safety and efficacy of glimepiride in patients with fair diabetic control (HbA1c level: 6.5-7.9%) have not been investigated so far. Therefore, we investigated the safety and efficacy of glimepiride titration using self-monitoring blood glucose (SMBG) in the achievement of strict glycemic control in fairly controlled diabetic patients. Japanese type 2 diabetic patients who were diet-controlled or treated with alpha-glucosidase inhibitor or metformin, were randomly assigned into the SMBG group with titration of glimepiride using SMBG, or the conventional therapy group (control group) without SMBG. Glimepiride was initiated at a dose of 0.5 mg/day and plasma glucose, insulin, HbA1c, and glycoalbumin levels were evaluated for 6 months in both groups. The dose of glimepiride was titrated in the SMBG group according to the SMBG levels before breakfast and dinner. The mean dose of glimepiride at 6 months tended to be higher in the SMBG than the control group (1.0±0.8 vs 0.6±0.3mg/day), but not significant. At 6 months after glimepiride treatment, HbA1c levels were significantly lower than at baseline (SMBG: 7.2±0.5 vs 6.5±0.6%, n=23, P<0.01, control: 7.3±0.4 vs 6.5±0.7%, n=24, P<0.01), although they were similar at 6 months in the two groups. Only three hypoglycemic episodes were recorded among 50 subjects. We found no efficacy of glimepiride titration protocol in this study. However, glimepiride significantly improved glycemic control in fairly controlled diabetic patients without severe hypoglycemia.
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