The role of glucagon-like peptide 1 in the postprandial effects of metformin in type 2 diabetes: a randomized crossover trial.

IF 5.3 1区医学 Q1 ENDOCRINOLOGY & METABOLISM

European Journal of Endocrinology Pub Date : 2024-08-05 DOI:10.1093/ejendo/lvae095

Laura S Hansen, Lærke S Gasbjerg, Andreas Brønden, Niels B Dalsgaard, Emilie Bahne, Signe Stensen, Pernille H Hellmann, Jens F Rehfeld, Bolette Hartmann, Nicolai J Wewer Albrechtsen, Jens J Holst, Tina Vilsbøll, Filip K Knop

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引用次数: 0

Abstract

Aims: Although metformin is widely used for treatment of type 2 diabetes (T2D), its glucose-lowering mechanism remains unclear. Using the glucagon-like peptide 1 (GLP-1) receptor (GLP-1R) antagonist exendin(9-39)NH2, we tested the hypothesis that postprandial GLP-1-mediated effects contribute to the glucose-lowering potential of metformin in T2D.

Methods: In a randomized, placebo-controlled, double-blind, crossover study, 15 individuals with T2D (median HbA1c 50 mmol/mol [6.7%], body mass index 30.1 kg/m2, age 71 years) underwent, in randomized order, 14 days of metformin and placebo treatment, respectively. Each treatment period was preceded by 14 days without any glucose-lowering medicine and concluded by two 4 h mixed meal tests performed in randomized order and separated by >24 h with either continuous intravenous exendin(9-39)NH2 or saline infusion.

Results: Compared to placebo, metformin treatment lowered fasting plasma glucose (mean of differences [MD] 1.4 mmol/L × min [95% CI 0.8-2.0]) as well as postprandial plasma glucose excursions during both saline infusion (MD 186 mmol/L × min [95% CI 64-307]) and exendin(9-39)NH2 infusion (MD 268 mmol/L × min [95% CI 108-427]). The metformin-induced improvement in postprandial glucose tolerance was unaffected by GLP-1R antagonization (MD 82 mmol/L × min [95% CI -6564-170]). Metformin treatment increased fasting plasma GLP-1 (MD 1.7 pmol/L × min [95% CI 0.39-2.9]) but did not affect postprandial GLP-1 responses (MD 820 pmol/L × min [95% CI -1750-111]).

Conclusions: Using GLP-1R antagonization, we could not detect GLP-1-mediated postprandial glucose-lowering effect of metformin in individuals with T2D. We show that 2 weeks of metformin treatment increases fasting plasma GLP-1, which may contribute to metformin's beneficial effect on fasting plasma glucose in T2D. Trial registration: Clinicaltrials.gov NCT03246451.

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胰高血糖素样肽 1 在二甲双胍对 2 型糖尿病患者的餐后效应中的作用：随机交叉试验。

目的：虽然二甲双胍被广泛用于治疗2型糖尿病（T2D），但其降糖机制仍不清楚。我们利用胰高血糖素样肽 1（GLP-1）受体（GLP-1R）拮抗剂 exendin(9-39)NH2，测试了餐后 GLP-1 介导的效应有助于二甲双胍在 T2D 中发挥降糖潜力的假设：在一项随机、安慰剂对照、双盲、交叉研究中，15 名 T2D 患者（中位 HbA1c 50 mmol/mol (6.7%)，体重指数 30.1 kg/m2，年龄 71 岁）按随机顺序分别接受了为期 14 天的二甲双胍和安慰剂治疗。每个治疗期之前的 14 天不服用任何降糖药物，治疗结束后按随机顺序进行两次 4 小时混合餐试验，试验间隔时间大于 24 小时，试验期间持续静脉输注二甲双胍（9-39）NH2 或生理盐水：结果：与安慰剂相比，二甲双胍治疗降低了空腹血浆葡萄糖（差异平均值 (MD) 1.4 mmol/l×min（95% CI 0.8-2.0）），以及在输注生理盐水（MD 186 mmol/l×min（95% CI 64-307））和输注依那西汀（9-39）NH2（MD 268 mmol/l×min（95% CI 108-427））时的餐后血浆葡萄糖偏移。二甲双胍诱导的餐后糖耐量改善不受 GLP-1R 拮抗的影响（MD 82 mmol/l×min（95% CI -6564-170））。二甲双胍治疗可增加空腹血浆 GLP-1（MD 1.7 pmol/l×min (95% CI 0.39-2.9)），但不影响餐后 GLP-1 反应（MD 820 pmol/l×min (95% CI -1,750-111) ）：结论：使用 GLP-1R 拮抗剂，我们无法检测到二甲双胍对 T2D 患者有 GLP-1 介导的餐后降糖作用。我们的研究表明，二甲双胍治疗两周可增加空腹血浆 GLP-1，这可能是二甲双胍对 T2D 患者空腹血浆葡萄糖产生有益影响的原因：试验注册：Clinicaltrials.gov NCT03246451。

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来源期刊

European Journal of Endocrinology 医学-内分泌学与代谢

CiteScore

9.80

自引率

3.40%

发文量

354

审稿时长

1 months

期刊介绍： European Journal of Endocrinology is the official journal of the European Society of Endocrinology. Its predecessor journal is Acta Endocrinologica. The journal publishes high-quality original clinical and translational research papers and reviews in paediatric and adult endocrinology, as well as clinical practice guidelines, position statements and debates. Case reports will only be considered if they represent exceptional insights or advances in clinical endocrinology. Topics covered include, but are not limited to, Adrenal and Steroid, Bone and Mineral Metabolism, Hormones and Cancer, Pituitary and Hypothalamus, Thyroid and Reproduction. In the field of Diabetes, Obesity and Metabolism we welcome manuscripts addressing endocrine mechanisms of disease and its complications, management of obesity/diabetes in the context of other endocrine conditions, or aspects of complex disease management. Reports may encompass natural history studies, mechanistic studies, or clinical trials. Equal consideration is given to all manuscripts in English from any country.