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健康男性经口和经十二指肠给予奎宁对混合营养素饮料血糖反应的比较影响:与糖调节激素和胃排空的关系。

Comparative Effects of Intragastric and Intraduodenal Administration of Quinine on the Plasma Glucose Response to a Mixed-Nutrient Drink in Healthy Men: Relations with Glucoregulatory Hormones and Gastric Emptying.

机构信息

Adelaide Medical School and Centre of Research Excellence in Translating Nutritional Science to Good Health, University of Adelaide, Adelaide, South Australia 5000, Australia.

Endocrine and Metabolic Unit, Royal Adelaide Hospital, Adelaide, Australia.

出版信息

J Nutr. 2021 Jun 1;151(6):1453-1461. doi: 10.1093/jn/nxab020.

Abstract

BACKGROUND

In preclinical studies, bitter compounds, including quinine, stimulate secretion of glucoregulatory hormones [e.g., glucagon-like peptide-1 (GLP-1)] and slow gastric emptying, both key determinants of postprandial glycemia. A greater density of bitter-taste receptors has been reported in the duodenum than the stomach. Thus, intraduodenal (ID) delivery may be more effective in stimulating GI functions to lower postprandial glucose.

OBJECTIVE

We compared effects of intragastric (IG) and ID quinine [as quinine hydrochloride (QHCl)] administration on the plasma glucose response to a mixed-nutrient drink and relations with gastric emptying, plasma C-peptide (reflecting insulin secretion), and GLP-1.

METHODS

Fourteen healthy men [mean ± SD age: 25 ± 3 y; BMI (in kg/m2): 22.5 ± 0.5] received, on 4 separate occasions, in double-blind, randomly assigned order, 600 mg QHCl or control, IG or ID, 60 min (IG conditions) or 30 min (IG conditions) before a mixed-nutrient drink. Plasma glucose (primary outcome) and hormones were measured before, and for 2 h following, the drink. Gastric emptying of the drink was measured using a 13C-acetate breath test. Data were analyzed using repeated-measures 2-way ANOVAs (factors: treatment and route of administration) to evaluate effects of QHCl alone and 3-way ANOVAs (factors: treatment, route-of-administration, and time) for responses to the drink.

RESULTS

After QHCl alone, there were effects of treatment, but not route of administration, on C-peptide, GLP-1, and glucose (P < 0.05); QHCl stimulated C-peptide and GLP-1 and lowered glucose concentrations (IG control: 4.5 ± 0.1; IG-QHCl: 3.9 ± 0.1; ID-control: 4.6 ± 0.1; ID-QHCl: 4.2 ± 0.1 mmol/L) compared with control. Postdrink, there were treatment × time interactions for glucose, C-peptide, and gastric emptying, and a treatment effect for GLP-1 (all P < 0.05), but no route-of-administration effects. QHCl stimulated C-peptide and GLP-1, slowed gastric emptying, and reduced glucose (IG control: 7.2 ± 0.3; IG-QHCl: 6.2 ± 0.3; ID-control: 7.2 ± 0.3; ID-QHCl: 6.4 ± 0.4 mmol/L)  compared with control.

CONCLUSIONS

In healthy men, IG and ID quinine administration similarly lowered plasma glucose, increased plasma insulin and GLP-1, and slowed gastric emptying. These findings have potential implications for lowering blood glucose in type 2 diabetes. This study was registered as a clinical trial with the Australian New Zealand Clinical Trials at www.anzctr.org.au as ACTRN12619001269123.

摘要

背景

在临床前研究中,苦味化合物(如奎宁)刺激糖调节激素(如胰高血糖素样肽-1(GLP-1))的分泌并减缓胃排空,这两者都是餐后血糖的关键决定因素。已有报道称十二指肠内的苦味受体密度高于胃。因此,十二指肠内(ID)给药可能更有效地刺激胃肠道功能以降低餐后血糖。

目的

我们比较了胃内(IG)和 ID 奎宁(作为盐酸奎宁(QHCl))给药对混合营养饮料引起的血浆葡萄糖反应的影响,以及与胃排空、血浆 C 肽(反映胰岛素分泌)和 GLP-1 的关系。

方法

14 名健康男性(平均年龄±标准差:25±3 岁;BMI(kg/m2):22.5±0.5)在 4 次单独的试验中,分别以双盲、随机顺序接受 600 mg QHCl 或对照,IG 或 ID,60 分钟(IG 条件)或 30 分钟(IG 条件),然后饮用混合营养饮料。在饮用前和饮用后 2 小时测量血浆葡萄糖(主要结局)和激素。使用 13C-乙酸盐呼气试验测量饮料的胃排空情况。使用重复测量 2 因素方差分析(因素:治疗和给药途径)来评估 QHCl 单独的作用,使用 3 因素方差分析(因素:治疗、给药途径和时间)来评估对饮料的反应。

结果

在 QHCl 单独给药后,治疗有影响,但给药途径没有影响,C 肽、GLP-1 和葡萄糖(P<0.05);与对照相比,QHCl 刺激 C 肽和 GLP-1 并降低葡萄糖浓度(IG 对照:4.5±0.1;IG-QHCl:3.9±0.1;ID 对照:4.6±0.1;ID-QHCl:4.2±0.1mmol/L)。在饮用后,葡萄糖、C 肽和胃排空存在治疗与时间的交互作用,GLP-1 存在治疗作用(均 P<0.05),但没有给药途径作用。QHCl 刺激 C 肽和 GLP-1,减缓胃排空,降低血糖(IG 对照:7.2±0.3;IG-QHCl:6.2±0.3;ID 对照:7.2±0.3;ID-QHCl:6.4±0.4mmol/L)与对照相比。

结论

在健康男性中,IG 和 ID 奎宁给药同样降低了血浆葡萄糖,增加了血浆胰岛素和 GLP-1,并减缓了胃排空。这些发现可能对 2 型糖尿病患者的血糖降低有影响。本研究在澳大利亚和新西兰临床试验网站(www.anzctr.org.au)作为 ACTRN12619001269123 进行了临床试验注册。

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