Issue 46, 2023, Issue in Progress

Design of electron-donating group substituted 2-PAM analogs as antidotes for organophosphate insecticide poisoning

Abstract

The use of organophosphate (OPs) pesticides is widespread in agriculture and horticulture, but these chemicals can be lethal to humans, causing fatalities and deaths each year. The inhibition of acetylcholinesterase (AChE) by OPs leads to the overstimulation of cholinergic receptors, ultimately resulting in respiratory arrest, seizures, and death. Although 2-pralidoxime (2-PAM) is the FDA-approved drug for treating OP poisoning, there is difficulty in blood–brain barrier permeation. To address this issue, we designed and evaluated a series of 2-PAM analogs by substituting electron-donating groups on the para and/or ortho positions of the pyridinium core using in silico techniques. Our PCM-ONIOM2 (MP2/6-31G*:PM7//B3LYP/6-31G*:UFF) binding energy results demonstrated that 13 compounds exhibited higher binding energy than 2-PAM. The analog with phenyl and methyl groups substituted on the para and ortho positions, respectively, showed the most favorable binding characteristics, with aromatic residues in the active site (Y124, W286, F297, W338, and Y341) and the catalytic residue S203 covalently bonding with paraoxon. The results of DS-MD simulation revealed a highly favorable apical conformation of the potent analog, which has the potential to enhance reactivation of AChE. Importantly, newly designed compound demonstrated appropriate drug-likeness properties and blood–brain barrier penetration. These results provide a rational guide for developing new antidotes to treat organophosphate insecticide toxicity.

Graphical abstract: Design of electron-donating group substituted 2-PAM analogs as antidotes for organophosphate insecticide poisoning

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Article information

Article type
Paper
Submitted
09 May 2023
Accepted
27 Sep 2023
First published
02 Nov 2023
This article is Open Access
Creative Commons BY license

RSC Adv., 2023,13, 32266-32275

Design of electron-donating group substituted 2-PAM analogs as antidotes for organophosphate insecticide poisoning

N. Kongkaew, K. Hengphasatporn, Y. Injongkol, P. Mee-udorn, L. Shi, P. Mahalapbutr, P. Maitarad, R. Harada, Y. Shigeta, T. Rungrotmongkol and A. S. Vangnai, RSC Adv., 2023, 13, 32266 DOI: 10.1039/D3RA03087C

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