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Synthesis, kinetic evaluation and molecular docking studies of donepezil-based acetylcholinesterase inhibitors.

Journal of molecular structure (2022-03-01)
Makar Makarian, Michael Gonzalez, Stephanie M Salvador, Shahrokh Lorzadeh, Paula K Hudson, Stevan Pecic
RESUMEN

In an effort to develop new therapeutic agents to treat Alzheimer's disease, a series of donepezil-based analogs were designed, synthesized using an environmentally friendly route, and biologically evaluated for their inhibitory activity against electric eel acetylcholinesterase (AChE) enzyme. In vitro studies revealed that the phenyl moiety of donepezil can be successfully replaced with a pyridine ring leading to equally potent inhibitors of electric eel AChE. Further kinetic evaluations of the most potent inhibitor showed a dual-binding (mixed inhibition) mode, similar to donepezil. Molecular modeling studies suggest that several additional residues could be involved in the binding of this inhibitor in the human AChE enzyme active site compared to donepezil.

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Sigma-Aldrich
Acetilcolinesterasa from Electrophorus electricus (electric eel), Type VI-S, lyophilized powder, 200-1,000 units/mg protein