通过两种药代动力学原器的协同作用,实现每月一次的胰岛素治疗:Fc 结合和脂肪酸酰化

IF 4.2 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Alexander N. Zaykov, Vasily M. Gelfanov, Tina M. Tagmose, Damien Demozay, Valentina Manfè, Rebecca Rohlfs, Marita Rivir, Diego Perez-Tilve, Brian Finan and Richard D. DiMarchi
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引用次数: 0

摘要

通过结合两种旨在延长血浆半衰期的不同策略:脂肪酸酰化和 Fc 结合,可以显著延长药物的药代动力学特性和治疗作用持续时间。我们以胰岛素为例进行了研究,结果表明,与仅含 Fc 的同类药物相比,双重延长的胰岛素类似物可大幅延长药效学效应,从而降低 STZ 治疗小鼠的血糖。在大鼠和狗模型中进行的直接药代动力学测量进一步证实了这种增强作用,证明了每月一次胰岛素治疗的潜力。研究结果表明,这种方法可广泛应用于各种基于肽和蛋白质的疗法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Toward once-monthly insulin therapy via synergy in two pharmacokinetic protractors: Fc-conjugation and fatty acid acylation†

Toward once-monthly insulin therapy via synergy in two pharmacokinetic protractors: Fc-conjugation and fatty acid acylation†

Toward once-monthly insulin therapy via synergy in two pharmacokinetic protractors: Fc-conjugation and fatty acid acylation†

Pharmacokinetic properties and duration of therapeutic action of a pharmaceutical agent can be significantly extended through the combination of two distinct strategies aimed at increasing plasma half-life: fatty acid acylation and Fc-conjugation. Using insulin as a case study, we demonstrate that a doubly protracted insulin analog produces a substantial prolongation of pharmacodynamic effect to lower blood glucose in STZ-treated mice when compared to the Fc-only counterparts. This enhancement is further corroborated by direct pharmacokinetic measurements in rat and dog models, demonstrating the potential for once-monthly insulin therapy. The results suggest that this approach might have broad application across a diverse spectrum of peptide- and protein-based therapeutics.

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CiteScore
6.10
自引率
0.00%
发文量
128
审稿时长
10 weeks
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