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二甲双胍单药治疗的临床继发失效。

Secondary failure of metformin monotherapy in clinical practice.

机构信息

Kaiser Permanente Center for Health Research, Portland, Oregon, USA.

出版信息

Diabetes Care. 2010 Mar;33(3):501-6. doi: 10.2337/dc09-1749. Epub 2009 Dec 29.

Abstract

OBJECTIVE We sought to document the secondary failure rate of metformin monotherapy in a clinical practice setting and to explore factors that predict therapeutic failure. RESEARCH DESIGN AND METHODS We studied 1,799 type 2 diabetic patients who, between 2004 and 2006, lowered their A1C to <7% after initiating metformin monotherapy as their first-ever anti-hyperglycemic drug. We examined all A1C values recorded through 31 December 2008 (2-5 years of follow-up), defining secondary failure as a subsequent A1C > or =7.5% or the addition or substitution of another anti-hyperglycemic agent. We used logistic regression to identify factors associated with the probability of secondary failure. RESULTS Of the 1,799 patients studied, 42% (n = 748) experienced secondary failure; the mean failure rate was 17% per year. However, patients who initiated metformin within 3 months of diabetes diagnosis failed at an age-and A1C-adjusted rate of 12.2% (10.5-14.4%) per year, and patients who initiated while A1C was <7% failed at an adjusted rate of 12.3% per year. An interaction term between duration of diagnosed diabetes and A1C was not significant. Age, duration, and A1C at initiation were the only factors that predicted secondary failure. CONCLUSIONS Although metformin failure may occur more rapidly in clinical practice than in clinical trails, initiating it soon after diabetes diagnosis and while A1C is low might preserve beta-cell function, prolong the effectiveness of metformin, reduce lifetime glycemic burden, and prevent diabetes complications. Our findings support the current treatment algorithm for hyperglycemia management that recommends metformin initiation when diabetes is first diagnosed.

摘要

目的 我们旨在记录二甲双胍单药治疗在临床实践环境中的继发失效率,并探讨预测治疗失败的因素。

研究设计和方法 我们研究了 1799 例 2 型糖尿病患者,他们在 2004 年至 2006 年间首次使用二甲双胍作为降糖药物,将糖化血红蛋白(A1C)降至<7%。我们检查了截至 2008 年 12 月 31 日(2-5 年的随访)记录的所有 A1C 值,将随后的 A1C≥7.5%或添加或替换另一种降糖药物定义为继发失败。我们使用逻辑回归来确定与继发失败概率相关的因素。

结果 在研究的 1799 例患者中,有 42%(n=748)发生了继发失败;平均失败率为每年 17%。然而,在糖尿病诊断后 3 个月内开始使用二甲双胍的患者,在年龄和 A1C 调整后的年失败率为 12.2%(10.5-14.4%),而在 A1C<7%时开始使用二甲双胍的患者,在年龄和 A1C 调整后的年失败率为 12.3%。诊断糖尿病的持续时间和 A1C 之间的交互项不显著。年龄、起始时的持续时间和 A1C 是唯一预测继发失败的因素。

结论 尽管二甲双胍在临床实践中的失效速度可能快于临床试验,但在糖尿病诊断后尽快开始使用二甲双胍,同时 A1C 较低,可能会保留β细胞功能,延长二甲双胍的有效性,降低终生血糖负担,并预防糖尿病并发症。我们的发现支持当前的高血糖管理治疗算法,即在首次诊断糖尿病时推荐使用二甲双胍。

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