Winzeler Bettina, da Conceição Ismael, Refardt Julie, Sailer Clara O, Dutilh Gilles, Christ-Crain Mirjam
Department of Endocrinology, Diabetology and Metabolism, University Hospital Basel, Basel, Switzerland.
Department of Clinical Research, University Hospital Basel, Basel, Switzerland.
Endocrine. 2020 Nov;70(2):292-298. doi: 10.1007/s12020-020-02394-2. Epub 2020 Jul 4.
Glucagon-like peptide-1 (GLP-1) receptor agonists (RA) reduce appetite and energy intake. Recent findings from animal studies suggest a role of GLP-1 in drinking and water homeostasis. We aimed to elucidate whether GLP-1 RA reduce fluid intake in healthy volunteers.
Double-blind, randomized, placebo-controlled, crossover study. 20 healthy volunteers received dulaglutide 1.5 mg and placebo (0,9% sodium chloride) subcutaneously once weekly for 3 weeks. At the end of each treatment period, participants attended an 8-h evaluation visit, during which they were requested to eat two standardized meals and to drink water ad libitum. The primary outcome was the total fluid intake (ml) during the evaluation visit.
Mean [SD] age of participants (60% female) was 27 [9.2] years. All but four participants drank less on dulaglutide versus placebo treatment despite identical food intake. The median [IQR] difference of fluid intake on dulaglutide compared to placebo treatment was -100 ml [-400-0]. Median [IQR] total fluid intake was 1300 ml [888-1600] versus 1600 ml [1000-1720], on dulaglutide and placebo treatment, p = 0.06. Median [IQR] 24-h urine output was reduced in dulaglutide versus placebo-treated participants: 1250 ml [975-2080] versus 1680 ml [1400-2040], p = 0.04. Median serum sodium levels were 140 mmol/L on both visits and no difference in thirst perception was noted.
GLP-1 RA such as dulaglutide seem to modulate fluid balance in humans. This leads us to speculate that GLP-1 RA may be an interesting therapeutic options for patients with excessive drinking behavior e.g., primary polydipsia.
胰高血糖素样肽-1(GLP-1)受体激动剂(RA)可降低食欲和能量摄入。动物研究的最新发现表明GLP-1在饮水和水稳态中起作用。我们旨在阐明GLP-1 RA是否会减少健康志愿者的液体摄入量。
双盲、随机、安慰剂对照、交叉研究。20名健康志愿者每周皮下注射一次度拉糖肽1.5mg和安慰剂(0.9%氯化钠),共3周。在每个治疗期结束时,参与者参加一次8小时的评估访视,在此期间他们被要求吃两顿标准化餐食并随意饮水。主要结局是评估访视期间的总液体摄入量(毫升)。
参与者的平均[标准差]年龄为27[9.2]岁(60%为女性)。尽管食物摄入量相同,但除4名参与者外,其余所有参与者在接受度拉糖肽治疗时的饮水量均低于接受安慰剂治疗时。与安慰剂治疗相比,度拉糖肽治疗时液体摄入量的中位数[四分位间距]差异为-100毫升[-400-0]。度拉糖肽和安慰剂治疗时的总液体摄入量中位数[四分位间距]分别为1300毫升[888-1600]和1600毫升[1000-1720],p = 0.06。与接受安慰剂治疗的参与者相比,接受度拉糖肽治疗的参与者24小时尿量中位数[四分位间距]减少:1250毫升[975-2080]对1680毫升[1400-2040],p = 0.04。两次访视时血清钠水平中位数均为140mmol/L,且未观察到口渴感有差异。
度拉糖肽等GLP-1 RA似乎可调节人体的液体平衡。这使我们推测,GLP-1 RA可能是治疗过度饮水行为患者(如原发性烦渴)的一个有趣的治疗选择。
