VU6007477,一种基于吡咯并[2,3 -]吡啶甲酰胺核心结构的新型M型PAM,无胆碱能不良事件。
VU6007477, a Novel M PAM Based on a Pyrrolo[2,3-]pyridine Carboxamide Core Devoid of Cholinergic Adverse Events.
作者信息
Engers Julie L, Childress Elizabeth S, Long Madeline F, Capstick Rory A, Luscombe Vincent B, Cho Hekyung P, Dickerson Jonathan W, Rook Jerri M, Blobaum Anna L, Niswender Colleen M, Engers Darren W, Conn P Jeffrey, Lindsley Craig W
机构信息
Vanderbilt Center for Neuroscience Drug Discovery, Department of Pharmacology, Department of Chemistry, Department of Biochemistry, and Vanderbilt Kennedy Center, School of Medicine, Vanderbilt University, Nashville, Tennessee 37232, United States.
出版信息
ACS Med Chem Lett. 2018 Sep 4;9(9):917-922. doi: 10.1021/acsmedchemlett.8b00261. eCollection 2018 Sep 13.
Abstract
Herein, we report the chemical optimization of a new series of M positive allosteric modulators (PAMs) based on a novel pyrrolo[2,3-]pyridine core, developed via scaffold hopping and iterative parallel synthesis. The vast majority of analogs in this series proved to display robust cholinergic seizure activity. However, by removal of the secondary hydroxyl group, VU6007477 resulted with good rat M PAM potency (EC = 230 nM, 93% ACh max), minimal M agonist activity (agonist EC > 10 μM), good CNS penetration (rat brain/plasma = 0.28, = 0.32; mouse = 0.16, = 0.18), and no cholinergic adverse events (AEs, e.g., seizures). This work demonstrates that within a chemical series prone to robust M ago-PAM activity, SAR can result, which affords pure M PAMs, devoid of cholinergic toxicity/seizure liability.
摘要
在此,我们报告了基于新型吡咯并[2,3 -]吡啶核心的一系列新型M正变构调节剂(PAMs)的化学优化,该系列通过骨架跃迁和迭代平行合成开发。该系列中的绝大多数类似物都显示出强大的胆碱能惊厥活性。然而,通过去除仲羟基,VU6007477具有良好的大鼠M PAM效力(EC = 230 nM,93% ACh最大值)、最小的M激动剂活性(激动剂EC > 10 μM)、良好的中枢神经系统渗透性(大鼠脑/血浆 = 0.28, = 0.32;小鼠 = 0.16, = 0.18),且无胆碱能不良事件(AEs,如惊厥)。这项工作表明,在一个易于产生强大的M ago - PAM活性的化学系列中,可以得到结构活性关系,从而提供不含胆碱能毒性/惊厥倾向的纯M PAMs。
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