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用氘改善代谢稳定性:强效、长效游离脂肪酸受体 1 激动剂 HWL-066 的发现。

Improving metabolic stability with deuterium: The discovery of HWL-066, a potent and long-acting free fatty acid receptor 1 agonists.

机构信息

Center of Drug Discovery, State Key Laboratory of Natural Medicines, China Pharmaceutical University, Nanjing, China.

School of Pharmacy, Guangdong Pharmaceutical University, Guangzhou, China.

出版信息

Chem Biol Drug Des. 2018 Aug;92(2):1547-1554. doi: 10.1111/cbdd.13321. Epub 2018 May 18.

Abstract

The free fatty acid receptor 1 (FFA1) is a potential target due to its function in enhancing of glucose-stimulated insulin secretion. The FFA1 agonist GW9508 has great potential for the treatment of type 2 diabetes mellitus, but it has been suffering from high plasma clearance probably because the phenylpropanoic acid is vulnerable to β-oxidation. To identify orally available analog without influence on the unique pharmacological mechanism of GW9508, we tried to interdict the metabolically labile group by incorporating two deuterium atoms at the α-position of phenylpropionic acid affording compound 4 (HWL-066). As expected, HWL-066 revealed a lower clearance (CL = 0.23 L  hr  kg ), higher maximum concentration (C  = 5907.47 μg/L), and longer half-life (T  = 3.50 hr), resulting in a 2.8-fold higher exposure than GW9508. Moreover, the glucose-lowering effect of HWL-066 was far better than that of GW9508 and comparable with TAK-875. Different from glibenclamide, no side-effect of hypoglycemia was observed in mice after oral administrating HWL-066 (80 mg/kg).

摘要

游离脂肪酸受体 1(FFA1)是一个潜在的靶点,因为它可以增强葡萄糖刺激的胰岛素分泌。FFA1 激动剂 GW9508 具有治疗 2 型糖尿病的巨大潜力,但由于苯丙酸易发生β氧化,其血浆清除率较高。为了寻找不影响 GW9508 独特药理学机制的可口服类似物,我们尝试在苯丙酸的α位引入两个氘原子来阻断代谢不稳定基团,得到化合物 4(HWL-066)。如预期的那样,HWL-066 表现出较低的清除率(CL=0.23 L/hr/kg)、更高的最大浓度(C=5907.47μg/L)和更长的半衰期(T=3.50hr),其暴露量是 GW9508 的 2.8 倍。此外,HWL-066 的降血糖效果远优于 GW9508,与 TAK-875 相当。与格列本脲不同,口服 HWL-066(80mg/kg)后在小鼠中未观察到低血糖的副作用。

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