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ADO09 是一种胰淀素类似物普兰林肽和胰岛素类似物 A21G 的复方制剂,与赖脯胰岛素相比,可降低 1 型糖尿病患者餐后血糖。

ADO09, a co-formulation of the amylin analogue pramlintide and the insulin analogue A21G, lowers postprandial blood glucose versus insulin lispro in type 1 diabetes.

机构信息

Profil, Neuss, Germany.

Adocia, Lyon, France.

出版信息

Diabetes Obes Metab. 2021 Apr;23(4):961-970. doi: 10.1111/dom.14302. Epub 2021 Jan 18.

Abstract

AIM

To compare the safety, pharmacokinetics and pharmacodynamics of ADO09 with insulin lispro (Lispro) and separate subcutaneous injections of human insulin and pramlintide (Ins&Pram) in 24 subjects with type 1 diabetes.

METHODS

At three dosing visits, participants received single doses of ADO09, Ins&Pram or Lispro immediately before eating a standardized mixed meal together with 1 g of acetaminophen, which was used as a surrogate marker to evaluate the kinetics of gastric emptying. Premeal blood glucose was adjusted to 126 mg/dL ± 10% by means of insulin and glucose infusions. The insulin dose was 7.5 U and the pramlintide dose was 45 μg. Blood glucose, glucagon and acetaminophen concentrations were assessed as pharmacodynamic endpoints; insulin and pramlintide concentrations were analysed as pharmacokinetic endpoints, and safety and tolerability were assessed.

RESULTS

Compared with Lispro, ADO09 reduced postprandial blood glucose (ppBG) excursions by more than 95% in the first hour postmeal (mean ± SD ∆AUC BG 0-1 h: 1.4 ± 9.9 mgh/dL vs. 43.5 ± 15.3 mgh/dL; p < .0001). Maximum ppBG was significantly improved with ADO09 (∆BGmax 87.0 ± 35.5 mg/dL) versus both Lispro (109.2 ± 31.1 mg/dL; p = .0133) and Ins&Pram (109.4 ± 44.3 mg/dL; p = .0357). Gastric emptying with ADO09 was similar to Ins&Pram and significantly slower than with Lispro. All treatments were well tolerated and both adverse events and hypoglycaemic events were rare during the meal test procedure.

CONCLUSION

ADO09 was well tolerated and markedly reduced ppBG compared with Lispro. ADO09 formulation was generally similar to the separate administration of insulin and pramlintide, except for a better BG level in the 4-8 h interval postmeal. These positive results warrant further investigations with ADO09.

摘要

目的

比较 ADO09 与赖脯胰岛素(Lispro)和皮下分别注射人胰岛素和普兰林肽(Ins&Pram)在 24 例 1 型糖尿病患者中的安全性、药代动力学和药效学。

方法

在三次给药访问中,参与者在进食标准混合餐后立即接受单剂量的 ADO09、Ins&Pram 或 Lispro,并服用 1 克对乙酰氨基酚作为评估胃排空动力学的替代标志物。餐前血糖通过胰岛素和葡萄糖输注调整至 126mg/dL±10%。胰岛素剂量为 7.5U,普兰林肽剂量为 45μg。血糖、胰高血糖素和对乙酰氨基酚浓度作为药效学终点进行评估;胰岛素和普兰林肽浓度作为药代动力学终点进行分析,并评估安全性和耐受性。

结果

与 Lispro 相比,ADO09 在餐后 1 小时内将餐后血糖(ppBG)波动降低了 95%以上(0-1 小时内的平均差值 AUC BG:1.4±9.9mgh/dL 与 43.5±15.3mgh/dL;p<0.0001)。ADO09 显著改善了最大餐后血糖(BGmax 87.0±35.5mg/dL),而 Lispro(109.2±31.1mg/dL;p=0.0133)和 Ins&Pram(109.4±44.3mg/dL;p=0.0357)。ADO09 的胃排空速度与 Ins&Pram 相似,显著慢于 Lispro。所有治疗均耐受良好,在进餐测试过程中,不良事件和低血糖事件均很少发生。

结论

ADO09 耐受性良好,与 Lispro 相比,显著降低了 ppBG。ADO09 制剂与单独使用胰岛素和普兰林肽总体相似,除了餐后 4-8 小时间隔的血糖水平更好。这些积极的结果表明需要进一步研究 ADO09。

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