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Effect of pramlintide on prandial glycemic excursions during closed-loop control in adolescents and young adults with type 1 diabetes

机译:普兰林肽对青少年1型糖尿病青少年闭环控制中餐时血糖偏移的影响

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OBJECTIVE - Even under closed-loop (CL) conditions, meal-related blood glucose (BG) excursions frequently exceed target levels as a result of delays in absorption of insulin from the subcutaneous site of infusion. We hypothesized that delaying gastric emptying with preprandial injections of pramlintide would improve postprandial glycemia by allowing a better match between carbohydrate and insulin absorptions. RESEARCH DESIGN AND METHODS - Eight subjects (4 female; age, 15-28 years; A1C, 7.5 6 0.7%) were studied for 48 h on a CL insulin-delivery system with a proportional integral derivative algorithm with insulin feedback: 24 h on CL control alone (CL) and 24 h on CL control plus 30-μg premeal injections of pramlintide (CLP). Target glucosewas set at 120 mg/dL; timing and contents of meals were identical on both study days. No premeal manual boluses were given. Differences in reference BG excursions, defined as the incremental glucose rise from premeal to peak, were compared between conditions for each meal. RESULTS - CLP was associated with overall delayed time to peak BG (2.5 ± 0.9 vs. 1.5 ± 0.5 h; P < 0.0001) and reduced magnitude of glycemic excursion (88 ± 42 vs. 113 ± 32 mg/dL; P = 0.006) compared with CL alone. Pramlintide effects on glycemic excursions were particularly evident at lunch and dinner, in association with higher premeal insulin concentrations at those mealtimes. CONCLUSIONS - Pramlintide delayed the time to peak postprandial BG and reduced the magnitude of prandial BG excursions. Beneficial effects of pramlintide on CL may in part be related to higher premeal insulin levels at lunch and dinner compared with breakfast.
机译:目的-即使在闭环(CL)条件下,由于从皮下注射部位吸收胰岛素的延迟,与餐有关的血糖(BG)偏移经常超过目标水平。我们假设通过餐前注射普兰林肽来延迟胃排空可以通过使碳水化合物与胰岛素吸收之间更好地匹配来改善餐后血糖。研究设计与方法-在具有胰岛素反馈的比例积分微分算法的CL胰岛素输送系统上,对8名受试者(4名女性;年龄在15-28岁; A1C:7.5 6 0.7%)进行了48小时的研究:单独的CL对照(CL)和24 h的CL对照加上30μg普兰林肽(CLP)的餐前注射。目标葡萄糖设定为120 mg / dL;在两个研究日中,进餐的时间和内容均相同。未给予餐前人工推注。在每餐的不同条件下,对参考BG偏移的差异(定义为从餐前到峰值的葡萄糖增量)进行了比较。结果-CLP与达到BG峰值的总体延迟时间(2.5±0.9 vs. 1.5±0.5 h; P <0.0001)和血糖波动幅度降低有关(88±42 vs. 113±32 mg / dL; P = 0.006)与仅CL相比。在午餐和晚餐时普兰林肽对血糖波动的影响尤为明显,这与那些进餐时间的餐前胰岛素浓度升高有关。结论:普兰林肽延迟了餐后血糖峰值的时间,并减少了餐后血糖波动的幅度。与早餐相比,普兰林肽对CL的有益作用可能与午餐和晚餐时餐前胰岛素水平升高有关。

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