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  2. Organoselenium Compounds as Acetylcholinesterase Inhibitors: Evidence and Mechanism of Mixed Inhibition

Organoselenium Compounds as Acetylcholinesterase Inhibitors: Evidence and Mechanism of Mixed Inhibition

  • J Phys Chem B. 2021 Feb 18;125(6):1531-1541. doi: 10.1021/acs.jpcb.0c08111.
Amit Kumawat 1 Shabnam Raheem 2 Fasil Ali 3 Tanveer Ali Dar 3 Suman Chakrabarty 1 Masood Ahmad Rizvi 2
Affiliations

Affiliations

  • 1 Department of Chemical, Biological & Macromolecular Sciences, S. N. Bose National Centre for Basic Sciences, Kolkata 700106, India.
  • 2 Department of Chemistry, University of Kashmir, Srinagar, 190006, Jammu and Kashmir, India.
  • 3 Department of Clinical Bio-Chemistry, University of Kashmir, Srinagar, 190006, Jammu and Kashmir, India.
Abstract

Acetylcholinesterase (AChE) inhibitors are actively used for the effective treatment of Alzheimer's disease. In recent years, the neuroprotective effects of organoselenium compounds such as ebselen and diselenides on the AChE activity have been investigated as potential therapeutic agents. In this work, we have carried out systematic kinetic and intrinsic fluorescence assays in combination with docking and molecular dynamics (MD) simulations to elucidate the molecular mechanism of the mixed inhibition of AChE by ebselen and diphenyl diselenide (DPDSe) molecules. Our MD simulations demonstrate significant heterogeneity in the binding modes and allosteric hotspots for DPDSe on AChE due to non-specific interactions. We have further identified that both ebselen and DPDSe can strongly bind around the peripheral anionic site (PAS), leading to non-competitive inhibition similar to other PAS-binding inhibitors. We also illustrate the entry of the DPDSe molecule into the gorge through a "side door", which offers an alternate entry point for AChE inhibitors as compared to the usual substrate entry point of the gorge. Together with results from experiments, these simulations provide mechanistic insights into the mixed type of inhibition for AChE using DPDSe as a promising inhibitor for AChE.

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