医学
阿卡波糖
卡格列净
餐后
安慰剂
内科学
交叉研究
随机对照试验
胃肠病学
2型糖尿病
内分泌学
药理学
胰岛素
外科
麻醉
糖尿病
替代医学
病理
作者
Carolina B. Lobato,Clara Tornoe Winding,Kirstine N. Bojsen‐Møller,Christoffer Martinussen,Simon Veedfald,Jens J. Holst,Sten Madsbad,Nils B. Jørgensen,Carsten Dirksen
摘要
Abstract Introduction Post‐bariatric hypoglycaemia (PBH) is a rare yet disabling clinical condition, mostly reported after Roux‐en‐Y gastric bypass (RYGB) surgery. RYGB is one of the most widely used and effective bariatric procedures. The pathophysiology of PBH remains unclear, and treatment options are limited in effectiveness and/or carry significant side effects. Acarbose slows carbohydrates digestion and absorption and is generally considered first‐line pharmacological treatment for PBH but its gastrointestinal side effects limit patient compliance. Canagliflozin inhibits intestinal and renal sodium‐dependent glucose absorption and reduces postprandial excursions of glucose, insulin and incretins after RYGB – effects that could be beneficial in ameliorating PBH. Aims The trial aims to investigate how blood glucose levels are affected during daily living in subjects with PBH during treatment with canagliflozin or acarbose compared with placebo, and to study the meal‐induced entero‐endocrine mechanisms implied in the treatment responses. Methods In a double‐blinded, randomized, crossover clinical trial, HypoBar I will investigate the effectiveness in reducing the risk of PBH, safety, ambulatory glucose profile and entero‐endocrine responses when PBH is treated with canagliflozin 300 mg twice daily during a 4‐week intervention period, compared with acarbose 50 mg thrice daily or placebo. Ethics and Dissemination HypoBar I is approved by the Local regulatory entities. Results will be published in peer‐reviewed journals. Conclusion If effective, well‐tolerated and safe, canagliflozin could be a novel treatment for people with PBH. HypoBar I might also unravel new mechanisms underlying PBH, potentially identifying new treatment targets. Trial Registration EudraCT number 2022–000157‐87.
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