Design, synthesis and preclinical evaluation of bio-conjugated amylinomimetic peptides as long-acting amylin receptor agonists

胰淀素 化学 胃排空 体内 硫醚 药理学 对乙酰氨基酚 皮下注射 口服 受体 内分泌学 内科学 糖尿病 生物化学 医学 立体化学 生物技术 小岛 生物
作者
Raymond J. Patch,Rui Zhang,Suzanne C. Edavettal,Mark J. Macielag,Annette Eckardt,Jiali Li,M. Rives,Wilson B. Edwards,Simon A. Hinke,Xi Qiu,Wenying Jian,Ondrej Libiger,Songmao Zheng,Jey Jeyaseelan,Yin Liang,Shamina M. Rangwala,James Leonard,Pamela J. Hornby
出处
期刊:European journal of medicinal chemistry [Elsevier BV]
卷期号:236: 114330-114330 被引量:3
标识
DOI:10.1016/j.ejmech.2022.114330
摘要

Pramlintide is an equipotent amylin analogue that reduces food intake and body weight in obese subjects and has been clinically approved as an adjunctive therapy for the treatment of adult diabetic patients. However, due to its extremely short half-life in vivo, a regimen of multiple daily administrations is required for achieving clinical effectiveness. Herein is described the development of prototypical long-acting pramlintide bioconjugates, in which pramlintide's disulfide-linked macrocycle was replaced by a cyclic thioether motif. This modification enabled stable chemical conjugation to a half-life extending antibody. In contrast to pramlintide (t1/2 < 0.75 h), bioconjugates 35 and 38 have terminal half-lives of ∼2 days in mice and attain significant exposure levels that are maintained up to 7 days. Single dose subcutaneous administration of 35 in lean mice, given 18-20 h prior to oral acetaminophen (AAP) administration, significantly reduced gastric emptying (as determined by plasma AAP levels). In a separate study, similar administration of 35 in fasted lean mice effected a reduction in food intake for up to 48 h. These data are consistent with durable amylinomimetic responses and provide the basis for further development of such long-acting amylinomimetic conjugates for the potential treatment of obesity and associated pathologies.
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