posted on 2023-01-05, 16:34authored byBharti Chauhan, Rajnish Kumar, Salahuddin, Himanshu Singh, Obaid Afzal, Abdulmalik Saleh
Alfawaz Altamimi, Mohd Mustaqeem Abdullah, Mohammad Shahar Yar, Mohamed Jawed Ahsan, Neeraj Kumar, Sanjay Kumar Yadav
In the presented manuscript, a new series of 2-[4-methoxy-3-(5-substituted
phenyl-[1,3,4]oxadiazol-2-ylmethoxy)-phenyl]-benzothiazoles (6a–n) have been synthesized and studied in
vivo and in silico for their anticonvulsant
potential. Maximum electroshocks (MES) and subcutaneous pentylenetetrazol
(scPTZ) models have been used for in vivo anticonvulsant
activity. Auto Dock 4.2 software was used for in silico studies, and the targeted protein was 5IOV.sThe antidepressant activity
of selected compounds (most active) was determined as a reduction
in locomotor activity through an actophotometer. In vivo and In silico studies proved that among all the
synthesized compounds, 6f, 6h, 6j, and 6l were the most potent with no neurotoxicity as compared to conventional
drugs (phenytoin and phenobarbital). The in silico studies also indicated about different binding interactions of synthetic
compounds to localize the binding receptors. The most likely mode
of action for these drugs, according to the docking analysis of active
compounds with various targets, is their binding to the VGCC and NMDA
receptors.