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A Selective andBrain Penetrant p38αMAPK InhibitorCandidate for Neurologic and Neuropsychiatric Disorders That AttenuatesNeuroinflammation and Cognitive Dysfunction

机译:选择性和脑渗透性p38αMAPK抑制剂减轻神经系统疾病和神经精神疾病的候选人神经炎症和认知功能障碍

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摘要

The p38αMAPK is a serine/threonine protein kinase and a key node in the intracellular signaling networks that transduce and amplify stress signals into physiological changes. A preponderance of preclinical data and clinical observations established p38αMAPK as a brain drug discovery target involved in neuroinflammatory responses and synaptic dysfunction in multiple degenerative and neuropsychiatric brain disorders. We summarize the discovery of highly selective, brain-penetrant, small molecule p38αMAPK inhibitors that are efficacious in diverse animal models of neurologic disorders. A crystallography and pharmacoinformatic approach to fragment expansion enabled the discovery of an efficacious hit. The addition of secondary pharmacology screens to refinement delivered lead compounds with improved selectivity, appropriate pharmacodynamics, and efficacy. Safety considerations and additional secondary pharmacology screens drove optimization that delivered the drug candidate MW01-18-150SRM (MW150), currently in early stage clinical trials.
机译:p38αMAPK是丝氨酸/苏氨酸蛋白激酶,是细胞内信号转导网络中的关键节点,可将压力信号转导并放大为生理变化。大量的临床前数据和临床观察证实,p38αMAPK是涉及多种退行性和神经精神性脑疾病的神经炎性反应和突触功能障碍的脑部药物发现靶标。我们总结了在多种神经疾病的动物模型中有效的高选择性,脑渗透性小分子p38αMAPK抑制剂的发现。晶体学和药物信息学方法用于片段扩展使得能够发现有效的命中。添加二级药理学筛选以改进选择性,合适的药效学和功效的铅化合物。安全性考虑因素和其他辅助药理学筛选推动了优化,该优化已交付了目前处于早期临床试验中的候选药物MW01-18-150SRM(MW150)。

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