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Rapid Computer Vision-Enabled Murine Screening System Identifies Neuropharmacological Potential of Two New Mechanisms

机译:快速的计算机视觉启用的小鼠筛查系统可确定两种新机制的神经药理学潜力

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摘要

The lack of predictive in vitro models for behavioral phenotypes impedes rapid advancement in neuropharmacology and psychopharmacology. In vivo behavioral assays are more predictive of activity in human disorders, but such assays are often highly resource-intensive. Here we describe the successful application of a computer vision-enabled system to identify potential neuropharmacological activity of two new mechanisms. The analytical system was trained using multiple drugs that are used clinically to treat depression, schizophrenia, anxiety, and other psychiatric or behavioral disorders. During blinded testing the PDE10 inhibitor TP-10 produced a signature of activity suggesting potential antipsychotic activity. This finding is consistent with TP-10’s activity in multiple rodent models that is similar to that of clinically used antipsychotic drugs. The CK1ε inhibitor PF-670462 produced a signature consistent with anxiolytic activity and, at the highest dose tested, behavioral effects similar to that of opiate analgesics. Neither TP-10 nor PF-670462 was included in the training set. Thus, computer vision-based behavioral analysis can facilitate drug discovery by identifying neuropharmacological effects of compounds acting through new mechanisms.
机译:行为表型的体外预测模型的缺乏阻碍了神经药理学和心理药理学的快速发展。体内行为分析更能预测人类疾病的活动,但此类分析通常需要大量资源。在这里,我们描述了计算机视觉支持系统的成功应用,以识别两种新机制的潜在神经药理活性。使用多种药物对分析系统进行了培训,这些药物在临床上用于治疗抑郁症,精神分裂症,焦虑症和其他精神病或行为障碍。在盲法测试中,PDE10抑制剂TP-10产生了活性信号,表明潜在的抗精神病活性。这一发现与TP-10在多种啮齿动物模型中的活性一致,类似于临床使用的抗精神病药。 CK1ε抑制剂PF-670462产生了与抗焦虑活性一致的特征,并且在测试的最高剂量下,其行为作用与阿片类镇痛药相似。 TP-10和PF-670462均未包含在培训集中。因此,基于计算机视觉的行为分析可以通过识别通过新机制起作用的化合物的神经药理作用来促进药物发现。

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