Bristol Myers Squibb Company, Research and Development, P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
J Med Chem. 2021 Mar 25;64(6):3086-3099. doi: 10.1021/acs.jmedchem.0c01878. Epub 2021 Mar 9.
Apelin-13 is an endogenous peptidic agonist of the apelin receptor (APJ) receptor with the potential for improving cardiac function in heart failure patients. However, the low plasma stability of apelin-13 necessitates continuous intravenous infusion for therapeutic use. There are several approaches to increase the stability of apelin-13 including attachment of pharmacokinetic enhancing groups, stabilized peptides, and Fc-fusion approaches. We sought a small-molecule APJ receptor agonist approach to target a compound with a pharmacokinetic profile amenable for chronic oral administration. This manuscript describes sequential optimization of the pyrimidinone series, leading to pyridinone , with potency equivalent to the endogenous ligand apelin-13 and with an excellent oral bioavailability and PK profile in multiple preclinical species. Compound exhibited robust pharmacodynamic effects similar to apelin-13 in an acute rat pressure-volume loop model and was advanced as a clinical candidate.
Apelin-13 是一种内源性肽类血管紧张素受体(APJ)激动剂,具有改善心力衰竭患者心功能的潜力。然而,apelin-13 的血浆稳定性低,需要连续静脉输注才能用于治疗。有几种方法可以提高 apelin-13 的稳定性,包括附着药代动力学增强基团、稳定肽和 Fc 融合方法。我们寻求一种小分子 APJ 受体激动剂方法,以靶向一种具有适合慢性口服给药的药代动力学特征的化合物。本文描述了嘧啶酮系列的顺序优化,导致了吡啶酮,其效价与内源性配体 apelin-13 相当,并且在多种临床前物种中具有优异的口服生物利用度和 PK 特征。化合物在急性大鼠压力-容积环模型中表现出与 apelin-13 相似的强大药效学作用,并被推进为临床候选药物。
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