Mzezewa_2021_J.Enzyme.Inhib.Med.Chem_36_1607

Reference

Title : Design, synthesis, and evaluation of 3,7-substituted coumarin derivatives as multifunctional Alzheimer's disease agents - Mzezewa_2021_J.Enzyme.Inhib.Med.Chem_36_1607
Author(s) : Mzezewa SC , Omoruyi SI , Zondagh LS , Malan SF , Ekpo OE , Joubert J
Ref : J Enzyme Inhib Med Chem , 36 :1607 , 2021
Abstract :

Multitarget directed ligands (MTDLs) are emerging as promising treatment options for Alzheimer's disease (AD). Coumarin derivatives serve as a good starting point for designing MTDLs due to their inherent inhibition of monoamine oxidase (MAO) and cholinesterase enzymes, which are complicit in AD's complex pathophysiology. A preliminary series of 3,7-substituted coumarin derivatives were synthesised and evaluated for enzyme inhibitory activity, cytotoxicity as well as neuroprotective ability. The results indicated that the compounds are weak cholinesterase inhibitors with five compounds demonstrating relatively potent inhibition and selectivity towards MAO-B with IC(50) values between 0.014 and 0.498 hx00B5;microM. Significant neuroprotective effects towards MPP(+)-compromised SH-SY5Y neuroblastoma cells were also observed, with no inherent cytotoxicity at 10 microM for all compounds. The overall results demonstrated that substitution of the phenylethyloxy moiety at the 7-position imparted superior general activity to the derivatives, with the propargylamine substitution at the 3-position, in particular, displaying the best MAO-B selectivity and neuroprotection.

PubMedSearch : Mzezewa_2021_J.Enzyme.Inhib.Med.Chem_36_1607
PubMedID: 34281458

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Citations formats

Mzezewa SC, Omoruyi SI, Zondagh LS, Malan SF, Ekpo OE, Joubert J (2021)
Design, synthesis, and evaluation of 3,7-substituted coumarin derivatives as multifunctional Alzheimer's disease agents
J Enzyme Inhib Med Chem 36 :1607

Mzezewa SC, Omoruyi SI, Zondagh LS, Malan SF, Ekpo OE, Joubert J (2021)
J Enzyme Inhib Med Chem 36 :1607