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二甲双胍联用磺脲类药物时的低血糖:一项系统评价和网状Meta分析

Hypoglycaemia when adding sulphonylurea to metformin: a systematic review and network meta-analysis.

作者信息

Andersen Stig Ejdrup, Christensen Mikkel

机构信息

Clinical Pharamcology Unit, Zealand University Hospital, DK-4000, Roskilde, Denmark.

Department of Clinical Pharmacology, Bispebjerg University Hospital, DK-2400, Copenhagen NV, Denmark.

出版信息

Br J Clin Pharmacol. 2016 Nov;82(5):1291-1302. doi: 10.1111/bcp.13059. Epub 2016 Aug 3.

Abstract

AIMS

The risk of hypoglycaemia may differ among sulphonylureas (SUs), but evidence from head-to-head comparisons is sparse. Performing a network meta-analysis to use indirect evidence from randomized controlled trials (RCTs), we compared the relative risk of hypoglycaemia with newer generation SUs when added to metformin.

METHODS

A systematic review identified RCTs lasting 12-52 weeks and evaluating SUs added to inadequate metformin monotherapy (≥1000 mg/day) in type 2 diabetes. Adding RCTs investigating the active comparators from the identified SU trials, we established a coherent network. Hypoglycaemia of any severity was the primary end point.

RESULTS

Thirteen trials of SUs and 14 of oral non-SU antihyperglycaemic agents (16 260 patients) were included. All reported hypoglycaemia only as adverse events. Producing comparable reductions in HbA of -0.66 to -0.84% (-7 to -9 mmol/mol), the risk of hypoglycaemia was lowest with gliclazide compared to glipizide (OR 0.22, CrI: 0.05 to 0.96), glimepiride (OR 0.40, CrI: 0.13 to 1.27), and glibenclamide (OR 0.21, CrI: 0.03 to 1.48). A major limitation is varying definitions of hypoglycaemia across studies.

CONCLUSIONS

When added to metformin, gliclazide was associated with the lowest risk of hypoglycaemia between the newer generation SUs. Clinicians should consider the risk of hypoglycaemia agent-specific when selecting an SU agent.

摘要

目的

磺脲类药物(SUs)导致低血糖的风险可能存在差异,但直接对比的证据较少。通过进行网状Meta分析以利用随机对照试验(RCT)的间接证据,我们比较了新一代SUs加用至二甲双胍时低血糖的相对风险。

方法

一项系统评价纳入了持续12 - 52周、评估SUs加用至二甲双胍单药治疗效果不佳(≥1000mg/天)的2型糖尿病患者的RCT。纳入已识别的SU试验中研究活性对照药的RCT,构建连贯的网状结构。任何严重程度的低血糖均为主要终点。

结果

纳入了13项SUs试验和14项口服非SU类降糖药试验(共16260例患者)。所有试验仅将低血糖作为不良事件报告。格列齐特、格列吡嗪、格列美脲和格列本脲降低糖化血红蛋白(HbA)的幅度相当(-0.66%至-0.84%,即-7至-9mmol/mol),但与格列吡嗪相比,格列齐特导致低血糖的风险最低(比值比[OR]0.22,可信区间[CrI]:0.05至0.96),与格列美脲相比风险为OR 0.40(CrI:0.13至1.27),与格列本脲相比风险为OR 0.21(CrI:0.03至1.48)。一个主要局限性是各研究对低血糖的定义不同。

结论

新一代SUs加用至二甲双胍时,格列齐特导致低血糖的风险最低。临床医生在选择SU类药物时应考虑特定药物导致低血糖的风险。

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本文引用的文献

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Hypoglycaemia, a global cause for concern.低血糖,一个全球关注的问题。
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