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Coumarin or benzoxazinone based novel carbonic anhydrase inhibitors: synthesis, molecular docking and anticonvulsant studies

机译:基于香豆素或苯并恶嗪酮的新型碳酸酐酶抑制剂:合成,分子对接和抗惊厥研究

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Abstract Among many others, coumarin derivatives are known to show human carbonic anhydrase (hCA) inhibitory activity. Since hCA inhibition is one of the underlying mechanisms that account for the activities of some antiepileptic drugs (AEDs), hCA inhibitors are expected to have anti-seizure properties. There are also several studies reporting compounds with an imidazole and/or benzimidazole moiety which exert these pharmacological properties. In this study, we prepared fifteen novel coumarin-bearing imidazolium and benzimidazolium chloride, nine novel benzoxazinone-bearing imidazolium and benzimidazolium chloride derivatives and evaluated their hCA inhibitory activities and along with fourteen previously synthesized derivatives we scanned their anticonvulsant effects. As all compounds inhibited purified hCA isoforms I and II, some of them also proved protective against Maximal electroshock seizure (MES) and ScMet induced seizures in mice. Molecular docking studies with selected coumarin derivatives have revealed that these compounds bind to the active pocket of the enzyme in a similar fashion to that previously described for coumarin derivatives.
机译:摘要在许多其他物质中,香豆素衍生物具有抑制人类碳酸酐酶(hCA)的活性。由于hCA抑制是解释某些抗癫痫药物(AED)活性的潜在机制之一,因此hCA抑制剂有望具有抗癫痫发作的特性。也有一些研究报道了具有咪唑和/或苯并咪唑部分的化合物具有这些药理特性。在这项研究中,我们制备了15种新颖的含香豆素的咪唑和氯化苯并咪唑鎓,9种新颖的含苯并嗪酮的咪唑和氯化苯并咪唑鎓衍生物并评估了它们的hCA抑制活性,并与14种先前合成的衍生物一起扫描了它们的抗惊厥作用。由于所有化合物均抑制纯化的hCA亚型I和II,因此其中一些还被证明具有抗小鼠最​​大电击惊厥(MES)和ScMet诱发的惊厥的保护作用。与选定的香豆素衍生物的分子对接研究表明,这些化合物以与先前描述的香豆素衍生物类似的方式结合到酶的活性口袋上。

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