New <scp>multitarget</scp> directed <scp>benzimidazole‐2‐thiol‐based</scp> heterocycles as prospective <scp>anti‐radical</scp> and <scp>anti‐Alzheimer</scp>'s agents
Abdul Latif, Samina Bibi, Sardar Ali, Ammara Ammara, Manzoor Ahmad, Ajmal Khan, Ahmed Al‐Harrasi, Farhat Ullah, Mumtaz Ali
Abstract
Abstract A series of new heterocycles ( 4 – 18 ) was synthesized by the structural modification of benzimidazole‐2‐thiol (BT, 2‐MBI). The structures of the synthesized compounds were confirmed with the help of high‐resolution mass spectrometry (HRMS) and 1 HNMR spectroscopy. High inhibitions of the oxidants such as ABTS and DPPH were observed for compounds 9 [IC 50 (s) = 167.4 μM (ABTS), 139.5 μM (DPPH)], 10 [IC 50 (s) = 186.5 μM (ABTS), 155.4 μM (DPPH)], 11 [IC 50 (s) = 286.1 μM (ABTS), 189.1 μM (DPPH)], 12 [IC 50 (s) = 310.8 μM (ABTS), 162.2 μM (DPPH)], 14 [IC 50 (s) = 281.3 μM (ABTS), 205.7 μM (DPPH)], 15 [IC 50 (s) = 284.1 μM (ABTS), 177.3 μM (DPPH)], and 16 [IC 50 (s) = 344.7 μM (ABTS), 270.2 μM (DPPH)] as compared with Ascorbic acid [IC 50 (s) = 340.9 μM (ABTS), 164.3 μM (DPPH)]. The anti‐Alzheimer's activity was performed in vitro against cholinesterase enzymes (AChE, BChE). Compound 11 was able to show significant inhibitions [IC 50 (s) = 121.2 μM (AChE), 38.3 μM (BChE)] as against that of galantamine [IC 50 (s) = 139.4 μM (AChE), 40.3 μM (BChE)]. Compound 14 was found as a very good inhibitor of butyrylcholinesterase (IC 50 = 35.4 μM) as compared with standard galantamine. Molecular docking was further performed to investigate the mechanism of anticholinesterase activity.