Monroy-Noyola_2021_Front.Biosci.(Landmark.Ed)_26_744

Reference

Title : Hydrolysis of chiral organophosphorus compounds by phosphotriesterases and mammalian paraoxonase-1 - Monroy-Noyola_2021_Front.Biosci.(Landmark.Ed)_26_744
Author(s) : Monroy-Noyola A , Almenares-Lopez D , Vilanova E
Ref : Front Biosci (Landmark Ed) , 26 :744 , 2021
Abstract :

Some organophosphorus compounds (OPs), which are used in the manufacturing of insecticides and nerve agents, are racemic mixtures with at least one chiral center with a phosphorus atom. Acute exposure of humans to these mixtures induces the covalent modification of acetylcholinesterase (AChE) and neuropathy target esterase (NTE) and causes a cholinergic syndrome or organophosphate-induced delayed polyneuropathy syndrome (OPIDP). These irreversible neurological effects are due to the stereoselective interaction of the racemic OPs with these B-esterases (AChE and NTE) and such interactions have been studied in vivo, ex vivo and in vitro, using stereoselective hydrolysis by A-esterases or phosphotriesterases (PTEs) and the PTE from Pseudomonas diminuta, and paraoxonase-1 (PON1) from mammalian serum. PON1 has a limited hydrolytic potential of the racemic OPs, while the bacterial PTE exhibits a significant catalytic activity on the less toxic isomers P(+) of the nerve agents. Avian serum albumin also shows a hydrolyzing capacity of chiral OPs with oxo and thio forms. There are ongoing environmental and bioremediation efforts to design and produce recombinants as bio-scavengers of OPs.

PubMedSearch : Monroy-Noyola_2021_Front.Biosci.(Landmark.Ed)_26_744
PubMedID: 33049692

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Citations formats

Monroy-Noyola A, Almenares-Lopez D, Vilanova E (2021)
Hydrolysis of chiral organophosphorus compounds by phosphotriesterases and mammalian paraoxonase-1
Front Biosci (Landmark Ed) 26 :744

Monroy-Noyola A, Almenares-Lopez D, Vilanova E (2021)
Front Biosci (Landmark Ed) 26 :744