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首页> 外文期刊>Progress in Artificial Intelligence >Pharmacokinetics and Pharmacodynamics of Insulin Tregopil in Relation to Premeal Dosing Time, Between Meal Interval, and Meal Composition in Patients With Type 2 Diabetes Mellitus
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Pharmacokinetics and Pharmacodynamics of Insulin Tregopil in Relation to Premeal Dosing Time, Between Meal Interval, and Meal Composition in Patients With Type 2 Diabetes Mellitus

机译:2型糖尿病患者膳食间隔与膳食组合物相关胰岛素Trepopil的药代动力学和药效学

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摘要

We evaluated the pharmacokinetics and pharmacodynamics of oral insulin tregopil in relation to premeal dosing time, between-meal interval, and meal composition type in type 2 diabetes mellitus patients in a randomized, placebo-controlled, crossover study consisting of 3 sequential cohorts. In Cohort 1, insulin tregopil administered 10 to 20 minutes before a meal resulted in optimal postmeal exposure and demonstrated better postprandial glucose-lowering effect (glucose area under concentration-time curve [AUC]) compared to the 30-minute group. In Cohort 2, insulin tregopil pharmacokinetic exposure (plasma AUC) showed a progressive increase through 4, 5, and 6 hours of between-meal interval. The 6-hour between-meal interval resulted in better absorption of insulin tregopil in comparison to 4- and 5-hour intervals. However, no significant differences were observed in pharmacodynamic parameters except for higher glucose AUC(0-180min) in the insulin tregopil 4-hour group during the afternoon meal as compared to the morning meal. In Cohort 3, a high-fiber meal had the least impact on insulin tregopil absorption and resulted in the highest reduction in plasma glucose levels in the afternoon. A high-fat meal reduced insulin tregopil absorption in the afternoon meal; however, pharmacodynamic response was not diminished significantly. Insulin tregopil has a rapid onset of action of approximately 10 minutes and, when administered 10 to 20 minutes before a meal, demonstrated up to 13% to 18% reduction in blood glucose levels compared to baseline. A 5-hour between-meal interval minimizes the impact of a meal on absorption of subsequent (afternoon) insulin tregopil dose, and the pharmacodynamic response of insulin tregopil is not altered by meal composition. Insulin tregopil was well tolerated in patients with type 2 diabetes mellitus.
机译:我们评估了口服胰岛素Trepopil的药代动力学和药效学与前膜给药时间,膳食间隔和膳食组成类型在2型糖尿病患者中,在由3个顺序队列组成的随机,安慰剂控制的交叉研究中,患有2型糖尿病患者。在Cohort 1中,胰岛素Trepopil在膳食前10至20分钟施用,导致最佳的蛋白质暴露,并展示了与30分钟组相比的更好的后葡萄糖降低效果(浓度 - 时间曲线[AUC]的葡萄糖面积)。在群组中,胰岛素Trecopil药代动力学暴露(血浆AUC)显示逐渐增加4,5和6小时的膳食间隔。与4-和5小时间隔相比,膳食间隔之间的6小时导致胰岛素Trepopil更好地吸收。然而,与早餐相比,在胰岛素Trepopil 4小时组中的高葡萄糖AUC(0-180min),除了高葡萄糖AUC(0-180min)之外,在药效学参数中没有观察到显着差异。在队列3中,高纤维膳食对胰岛素Tregopil吸收的影响最小,并导致下午的血浆葡萄糖水平的最高降低。午餐中的胰岛素Trepopil吸收降低了高脂肪餐;然而,药效学反应未显着减少。胰岛素Trepopil具有大约10分钟的速度快速发作,并且当在膳食前10至20分钟施用时,与基线相比,血糖水平的降低高达13%至18%。膳食间隔之间的5小时最小化了膳食对随后(下午)胰岛素Tregopil剂量的吸收的影响,并且胰岛素Trepopil的药效响应不会通过膳食组合物改变。胰岛素Tregopil在2型糖尿病患者中耐受良好。

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