Agha_2022_J.Enzyme.Inhib.Med.Chem_37_1241

Reference

Title : Novel Sunifiram-carbamate hybrids as potential dual acetylcholinesterase inhibitor and NMDAR co-agonist: simulation-guided analogue design and pharmacological screening - Agha_2022_J.Enzyme.Inhib.Med.Chem_37_1241
Author(s) : Agha KA , Abo-Dya NE , Issahaku AR , Agoni C , Soliman MES , Abdel-Aal EH , Abdel-Samii ZK , Ibrahim TS
Ref : J Enzyme Inhib Med Chem , 37 :1241 , 2022
Abstract :

An efficient method for synthesising NMDAR co-agonist Sunifiram (DM235), in addition to Sunifram-carbamate and anthranilamide hybrids, has been developed in high yields via protecting group-free stepwise unsymmetric diacylation of piperazine using N-acylbenzotiazole. Compounds 3f, 3d, and 3i exhibited promising nootropic activity by enhancing acetylecholine (ACh) release in A549 cell line. Moreover, the carbamate hybrid 3f was found to exhibit higher in vitro potency than donepezil with IC(50) = 18 +/- 0.2 nM, 29.9 +/- 0.15 nM for 3f and donepezil, respectively. 3f was also found to effectively inhibit AChE activity in rat brain (AChE = 1.266 ng/mL) compared to tacrine (AChE = 1.137 ng/ml). An assessment of the ADMET properties revealed that compounds 3f, 3d, and 3i are drug-like and can penetrate blood-brain barrier. Findings presented here showcase highly potential cholinergic agents, with expected partial agonist activity towards glycine binding pocket of NMDAR which could lead to development and optimisation of novel nootropic drugs.

PubMedSearch : Agha_2022_J.Enzyme.Inhib.Med.Chem_37_1241
PubMedID: 35484855

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Citations formats

Agha KA, Abo-Dya NE, Issahaku AR, Agoni C, Soliman MES, Abdel-Aal EH, Abdel-Samii ZK, Ibrahim TS (2022)
Novel Sunifiram-carbamate hybrids as potential dual acetylcholinesterase inhibitor and NMDAR co-agonist: simulation-guided analogue design and pharmacological screening
J Enzyme Inhib Med Chem 37 :1241

Agha KA, Abo-Dya NE, Issahaku AR, Agoni C, Soliman MES, Abdel-Aal EH, Abdel-Samii ZK, Ibrahim TS (2022)
J Enzyme Inhib Med Chem 37 :1241