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首页> 外文期刊>Journal of Medicinal Chemistry >From High-Throughput Screening to Target Validation: Benzo[d]isothiazoles as Potent and Selective Agonists of Human Transient Receptor Potential Cation Channel Subfamily M Member 5 Possessing In Vivo Gastrointestinal Prokinetic Activity in Rodents
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From High-Throughput Screening to Target Validation: Benzo[d]isothiazoles as Potent and Selective Agonists of Human Transient Receptor Potential Cation Channel Subfamily M Member 5 Possessing In Vivo Gastrointestinal Prokinetic Activity in Rodents

机译:从高通量筛选到靶向验证:苯并[D]异噻唑作为人类瞬态受体潜在阳离子通道亚家族M患者5具有啮齿动物中的体内胃肠动力活性的有效和选择性激动剂

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摘要

Transient receptor potential cation channel subfamily M member 5 (TRPM5) is a nonselective monovalent cation channel activated by intracellular Ca2+ increase. Within the gastrointestinal system, TRPM5 is expressed in the stoma, small intestine, and colon. In the search for a selective agonist of TRPM5 possessing in vivo gastrointestinal prokinetic activity, a high-throughput screening was performed and compound 1 was identified as a promising hit. Hit validation and hit to lead activities led to the discovery of a series of benzo[d]isothiazole derivatives. Among these, compounds 61 and 64 showed nanomolar activity and excellent selectivity (>100-fold) versus related cation channels. The in vivo drug metabolism and pharmacokinetic profile of compound 64 was found to be ideal for a compound acting locally at the intestinal level, with minimal absorption into systemic circulation. Compound 64 was tested in vivo in a mouse motility assay at 100 mg/kg, and demonstrated increased prokinetic activity.
机译:瞬时受体电位阳离子通道亚家族M成员5(TRPM5)是由细胞内Ca2+增加激活的非选择性单价阳离子通道。在胃肠系统内,TRPM5在造口、小肠和结肠中表达。在寻找具有体内胃肠促动力活性的TRPM5选择性激动剂的过程中,进行了高通量筛选,化合物1被确定为一个有希望的目标。点击验证和点击到铅的活动导致了一系列苯并[d]异噻唑衍生物的发现。其中,化合物61和64相对于相关阳离子通道显示出纳摩尔活性和优异的选择性(>100倍)。研究发现,化合物64的体内药物代谢和药代动力学特征对于在肠道水平局部发挥作用的化合物来说是理想的,其在体循环中的吸收最小。在100 mg/kg的小鼠运动试验中对化合物64进行了体内试验,并证明其促动活性增强。

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