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2型糖尿病与二甲双胍。单药治疗的首选:疗效证据不足,但不良反应众所周知且可接受。

Type 2 diabetes and metformin. First choice for monotherapy: weak evidence of efficacy but well-known and acceptable adverse effects.

出版信息

Prescrire Int. 2014 Nov;23(154):269-72.

Abstract

Many guidelines recommend metformin as first-line therapy for patients with type 2 diabetes. This recommendation is primarily based on the results of the Ukpds trial published in 1998. However, the methodology of this trial has been criticised. In 2014, does the harm-benefit balance of metformin still justify its first-line use in type 2 diabetes? To answer this question, we conducted a review of the literature using the standard Prescrire methodology. In the Ukpds trial, involving about 1700 overweight diabetic patients, metformin monotherapy for about 10 years was more effective in reducing mortality than glycaemic control based mainly on dietary measures, and also more effective than treatment with a sulphonylurea such as chlorpropamide or glibenclamide, or with insulin. However, these results are undermined by several methodological flaws. In the Adopt trial, in which about 4400 patients were followed for 4 years, metformin, glibenclamide and rosiglitazone did not have significantly different effects on the risk of death or cardiovascular events. A meta-analysis of ten randomised trials versus placebo or other hypoglycaemic drugs did not show that metformin monotherapy had a statistically significant effect on mortality. In the Cosmic trial, including more than 5000 patients, metformin monotherapy for one year was not more effective in reducing mortality than another oral hypoglycaemic drug. In the Spread-Dimcad trial in 304 diabetic patients with coronary artery disease, metformin monotherapy appeared to be more effective in preventing cardiovascular complications than glipizide after 5 years of follow-up. The adverse effects of metformin mainly consist of dose-dependent gastrointestinal disorders and rare cases or life-threatening lactic aciaosis. Kidney failure reduces metformin elimination. Metformin rarely causes hypoglycaemia and has no effect on body weight. It does not increase cancer-related mortality. It sometimes causes vitamin B12 deficiency leading to macrocytic anaemia or peripheral neuropathy. Metformin mainly carries a risk of interactions with drugs that impair renal function, such as non-steroidal anti-inflammatory drugs and iodinated contrast media. Renal failure can lead to metformin accumulation and an increased risk of lactic acidosis. In mid-2014, the only study to show a reduction in mortality and complications of diabetes remains the Ukpds trial. Taken together, the available data suggest that metformin monotherapy tends to reduce mortality and cardiovascular morbidity and mortality. Its adverse effects have been extensively studied and are acceptable provided renal function is monitored, especially in situations in which patients are at risk of kidney failure.The harm-benefit balance of metformin monotherapy remains favourable in most patients with type 2 diabetes when dietary measures alone are not sufficient.

摘要

许多指南推荐二甲双胍作为2型糖尿病患者的一线治疗药物。这一推荐主要基于1998年发表的英国前瞻性糖尿病研究(Ukpds)试验结果。然而,该试验的方法受到了批评。2014年,二甲双胍的利弊平衡是否仍能证明其在2型糖尿病中的一线应用合理性?为回答这个问题,我们采用标准的Prescrire方法对文献进行了综述。在Ukpds试验中,约1700名超重糖尿病患者参与,二甲双胍单药治疗约10年在降低死亡率方面比主要基于饮食措施的血糖控制更有效,也比使用磺脲类药物如氯磺丙脲或格列本脲或胰岛素治疗更有效。然而,这些结果受到几个方法学缺陷的影响。在ADOPT试验中,约4400名患者随访4年,二甲双胍、格列本脲和罗格列酮在死亡风险或心血管事件方面没有显著差异。一项针对与安慰剂或其他降糖药物对比的十项随机试验的荟萃分析未显示二甲双胍单药治疗对死亡率有统计学显著影响。在COSMIC试验中,纳入超过5000名患者,二甲双胍单药治疗一年在降低死亡率方面并不比另一种口服降糖药更有效。在304例冠心病糖尿病患者的SPREAD-DIMCAD试验中,随访5年后,二甲双胍单药治疗在预防心血管并发症方面似乎比格列吡嗪更有效。二甲双胍 的不良反应主要包括剂量依赖性胃肠道疾病以及罕见的或危及生命的乳酸性酸中毒。肾衰竭会减少二甲双胍的清除。二甲双胍很少引起低血糖,对体重没有影响。它不会增加癌症相关死亡率。它有时会导致维生素B12缺乏,进而导致巨幼细胞贫血或周围神经病变。二甲双胍主要存在与损害肾功能的药物相互作用的风险,如非甾体抗炎药和碘化造影剂。肾衰竭会导致二甲双胍蓄积,增加乳酸性酸中毒风险。在2014年年中,唯一显示能降低糖尿病死亡率和并发症的研究仍是Ukpds试验。综合来看,现有数据表明二甲双胍单药治疗倾向于降低死亡率以及心血管发病率和死亡率。其不良反应已得到广泛研究,只要监测肾功能,尤其是在患者有肾衰竭风险的情况下,这些不良反应是可以接受的。对于大多数仅靠饮食措施不足以控制病情的2型糖尿病患者,二甲双胍单药治疗的利弊平衡仍然有利。

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