Chemistry and Chemical Engineering Research Center of Iran (CCERCI), Tehran, Iran.
Cellular and Molecular Biology Research Center, Health Research Institute, Babol University of Medical Sciences, Babol, Iran.
J Biochem Mol Toxicol. 2023 Jan;37(1):e23234. doi: 10.1002/jbt.23234. Epub 2022 Oct 2.
A new series of spiro[indene-1,2'-quinazolin]-4'(3'H)-one derivatives 4a-m were synthesized via a one-pot method and evaluated for anticonvulsant activities using pentylenetetrazole (PTZ) and maximal electroshock (MES)-induced seizures. Obtained results demonstrated that these compounds have not anticonvulsant activity in PTZ test while are active in the MES test. Among the synthesized compounds, the best anticonvulsant activity was obtained with compound 4h. This compound also was not neurotoxic. Given that the title new compounds have the pharmacophore requirement for benzodiazepine (BZD) receptor agonist, the most potent compound was assayed in vivo and in silico as BZD receptor agonist. After treatment with flumazenil as a standard BZD receptor antagonist, anticonvulsant activity of compound 4h decreased. Therefore, the involvement of BZD receptors in anticonvulsant activity of this compound confirmed. Furthermore, docking study of compound 4h in the BZD-binding site of GABA receptor confirmed that this compound interacted with the important residues.
通过一锅法合成了一系列新的螺[茚并-1,2'-喹唑啉]-4'(3'H)-酮衍生物 4a-m,并使用戊四氮(PTZ)和最大电休克(MES)诱导的癫痫发作评估其抗惊厥活性。结果表明,这些化合物在 PTZ 试验中没有抗惊厥活性,而在 MES 试验中具有活性。在所合成的化合物中,化合物 4h 具有最佳的抗惊厥活性。该化合物也没有神经毒性。鉴于标题新化合物具有苯二氮䓬(BZD)受体激动剂的药效团要求,最有效的化合物在体内和体外作为 BZD 受体激动剂进行了检测。用氟马西尼作为标准 BZD 受体拮抗剂处理后,化合物 4h 的抗惊厥活性降低。因此,证实了该化合物的 BZD 受体参与其抗惊厥活性。此外,化合物 4h 在 GABA 受体的 BZD 结合位点的对接研究证实,该化合物与重要残基相互作用。
