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Anticholinesterase activity of some major intermediates in carbacylamidophosphate synthesis: Preparation,spectral characterization and inhibitory potency determination
Authors:Khodayar Gholivand  Ahlam Madani Alizadegan  Azam Anaraki Firooz  Khosro Khajeh  Hossein Naderi-manesh  Hamidreza Bijanzadeh
Institution:1. Faculty of Science, Tarbiat Modarres University, 1Department of Chemistry, P.O. Box: 14115-175, Tehran, Iran;2. Faculty of Science, Tarbiat Modarres University, 2Department of Biochemistry and Biophysics, Tehran, Iran
Abstract:Carbacylamidophosphates with the general formula RC(O)NHP(O)R1R2 constitute organophosphorus compounds that are used as insecticides, pesticides and ureas inhibitors. In this work, we studied the inhibition potency of CCl3C(O)NHP(O)Cl21, CHCl2C(O)NHP(O)Cl22, CH2ClC(O)NHP(O)Cl23 and CF3C(O)NHP(O)Cl24, which are the major intermediates for carbacylamidophosphates synthesis towards human erythrocyte acetylcholinesterase (hAChe) activity using Ellman's modified kinetic method. Unexpectedly, it was observed that they were not only hydrolytically unstable but also inhibited hAChE in a similar manner to that produced by organophosphorus insecticides. Enzymatic data, bimolecular inhibition rate constants (ki) and IC50 values for inhibition of hAChE demonstrated that they are irreversible inhibitors and the inhibition potency of compound 2 (IC50 = 88 μM) was the greatest in comparison with compounds 1, 3 and 4. Also the electropositivity of the phosphorus atom and the hydrophobicity of the compounds demonstrated that these two factors play an additional effect and different role in the inhibitory activity of these compounds. Hydrolytic stability of the compounds was determined by 31P NMR monitoring of the loss of the parent molecules with D2O as a function of time. This study considers antiacetylcholinesterase activity according to the structural and the electronic aspects of compounds 14, according to IR, 1H, 13C and 31P NMR spectral data.
Keywords:Carbacylamidophosphate  human erythrocytes acetylcholinesterase  hydrophobicity  IC50 value  irreversible inhibitor
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