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Acylated heptapeptide binds albumin with high affinity and application as tag furnishes long-acting peptides

机译:酰化的七肽以高亲和力结合白蛋白,并作为标签提供长效肽的应用

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摘要

The rapid renal clearance of peptides in vivo limits this attractive platform for the treatment of a broad range of diseases that require prolonged drug half-lives. An intriguing approach for extending peptide circulation times works through a ‘piggy-back’ strategy in which peptides bind via a ligand to the long-lived serum protein albumin. In accordance with this strategy, we developed an easily synthesized albumin-binding ligand based on a peptide-fatty acid chimera that has a high affinity for human albumin ( K d=39?nM). This ligand prolongs the elimination half-life of cyclic peptides in rats 25-fold to over seven hours. Conjugation to a peptide factor XII inhibitor developed for anti-thrombotic therapy extends the half-life from 13 minutes to over five hours, inhibiting coagulation for eight hours in rabbits. This high-affinity albumin ligand could potentially extend the half-life of peptides in human to several days, substantially broadening the application range of peptides as therapeutics.
机译:体内肽的快速肾脏清除限制了这个有吸引力的平台,可用于治疗需要延长药物半衰期的多种疾病。延长肽循环时间的一种有趣方法是通过“背负式”策略进行,在该策略中,肽通过配体与长寿的血清蛋白白蛋白结合。按照这种策略,我们开发了一种基于易于合成的多肽-脂肪酸配体,该配体对人白蛋白(K d = 39?nM)具有很高的亲和力。该配体将环肽在大鼠中的消除半衰期延长了25倍至7个小时以上。与开发用于抗血栓治疗的肽因子XII抑制剂的缀合可将半衰期从13分钟延长至超过5小时,从而在兔体内抑制凝血8小时。这种高亲和力的白蛋白配体可将肽在人体内的半衰期延长至数天,从而大大拓宽了肽作为治疗剂的应用范围。

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