VU6007477 a Novel M1 PAM Based on a Pyrrolo23-bpyridine Carboxamide Core Devoid of Cholinergic AdverseEvents

机译：VU6007477一种基于吡咯并23-b吡啶羧酰胺核的新型M1 PAM不含胆碱能不良药物大事记

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摘要

Herein, we report the chemical optimization of a new series of M1 positive allosteric modulators (PAMs) based on a novel pyrrolo[2,3-b]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 M1 PAM potency (EC50 = 230 nM, 93% ACh max), minimal M1 agonist activity (agonist EC50 > 10 μM), good CNS penetration (rat brain/plasma Kp = 0.28, Kp,uu = 0.32; mouse Kp = 0.16, Kp,uu = 0.18), and no cholinergic adverse events (AEs, e.g., seizures). This work demonstrates that within a chemical series prone to robust M1 ago-PAM activity, SAR can result, which affords pure M1 PAMs, devoid of cholinergic toxicity/seizure liability.

机译：在这里，我们报告了基于新型的吡咯并[2,3-b]吡啶核，通过骨架跳跃和迭代平行合成开发的一系列新的M1正构构调节剂（PAM）的化学优化。该系列中的绝大多数类似物证明具有强大的胆碱能癫痫发作活性。但是，通过除去仲羟基，VU6007477具有良好的大鼠M1 PAM效能（EC50 = 230 nM，ACh最大值为93％），最小的M1激动剂活性（激动剂EC50> 10μM），良好的CNS渗透（大鼠脑/血浆） Kp ＝ 0.28，Kp，uu ＝ 0.32；小鼠Kp ＝ 0.16，Kp，uu ＝ 0.18），并且没有胆碱能不良事件（AE，例如癫痫发作）。这项工作表明，在易于产生强效M1前PAM活性的化学系列中，可以产生SAR，从而提供了纯M1 PAM，没有胆碱能毒性/癫痫发作的责任。

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期刊名称 ACS Medicinal Chemistry Letters
作者
Julie L. Engers; Elizabeth S. Childress; Madeline F. Long; Rory A. Capstick; Vincent B. Luscombe; Hekyung P. Cho; Jonathan W. Dickerson; Jerri M. Rook; Anna L. Blobaum; Colleen M. Niswender; Darren W. Engers; P. Jeffrey Conn; Craig W. Lindsley; *;
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年(卷),期 2018(9),9
年度 2018
页码 917–922
总页数 6
原文格式 PDF
正文语种
中图分类药物化学;
关键词
Positive allosteric modulator (PAM) muscarinic acetylcholine receptor 1 (M1) cholinergic toxicity VU6007477;

机译：正变构调节剂（PAM）;毒蕈碱乙酰胆碱受体1（M1）;胆碱能毒性;VU6007477;

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专利

1. VU6007477, a Novel M-1 PAM Based on a Pyrrolo[2,3-b]pyridine Carboxamide Core Devoid of Cholinergic Adverse Events [J] . Engers Julie L., Childress Elizabeth S., Long Madeline F., ACS medicinal chemistry letters . 2018,第9期

机译：VU6007477，一种基于吡咯的新型M-1 PAM [2,3-B]吡啶甲酰胺核心缺乏胆碱能不良事件
2. Discovery of the Potent and Selective M1 PAM-Agonist N-[(3R,4S)-3-Hydroxytetrahydro-2H-pyran-4-yl]-5-methyl-4-[4-(1,3-thiazol-4-yl)benzyl]pyridine-2-carboxamide (PF-06767832): Evaluation of Efficacy and Cholinergic Side Effects [J] . Davoren Jennifer E., Lee Che-Wah, Garnsey Michelle, Journal of Medicinal Chemistry . 2016,第13期

机译：发现强而有选择性的M1 PAM激动剂N-[（3R，4S）-3-羟基四氢-2H-吡喃-4-基] -5-甲基-4- [4-（1,3-噻唑-4- （基）苄基]吡啶-2-甲酰胺（PF-06767832）：疗效和胆碱能副作用的评估
3. Cadmium-induced cell death of basal forebrain cholinergic neurons mediated by muscarinic M1 receptor blockade, increase in GSK-3 beta enzyme, beta-amyloid and tau protein levels [J] . del Pino Javier, Zeballos Gabriela, Jose Anadon Maria, Archives of Toxicology . 2016,第5期

机译：毒蕈碱M1受体阻滞介导的镉诱导的基础前脑胆碱能神经元细胞死亡，GSK-3β酶，β-淀粉样蛋白和tau蛋白水平的升高
4. Carrier Beating Impairment of PAM, CAP and DMT in Multicore Fiber Based IM/DD Systems [C] . Lin Gan, Jiajun Zhou, Ming Tang, Asia Communications and Photonics Conference . 2019

机译：基于多芯光纤的IM / DD系统中PAM，CAP和DMT的载波跳动损害
5. The discovery of VU0486846: steep SAR from a series of M1 PAMs based on a novel benzomorpholine core [O] . Jeanette L. Bertron, Hyekyung P. Cho, Pedro M. Garcia-Barrantes, -1

机译：VU0486846的发现：基于新型苯并吗啉核心的一系列M1 PAM的陡峭SAR
6. The discovery of VU0486846: steep SAR from a series of M1 PAMs based on a novel benzomorpholine core [O] . Jeanette L. Bertron, Hyekyung P. Cho, Pedro M. Garcia-Barrantes, 2018

机译：Vu0486846的发现：根据基于新型苯齐洛林核心的一系列M1 PAM陡峭的SAR

VU6007477 a Novel M1 PAM Based on a Pyrrolo23-bpyridine Carboxamide Core Devoid of Cholinergic AdverseEvents

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