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Structure-activity relationship on human serum paraoxonase (PON1) using substrate analogues and inhibitors
Authors:Bargota Rakesh S  Akhtar Mahmoud  Biggadike Keith  Gani David  Allemann Rudolf K
Institution:School of Chemical Sciences, The University of Birmingham, Edgbaston, UK.
Abstract:Substrate analogues based on the parent compounds paraoxon and phenyl acetate were tested on human serum paraoxonase (PON1) to explore the active site of the enzyme. Replacement of the nitro group of paraoxon with an amine or hydrogen, as well as electronic changes to the parent compound, converted these analogues into inhibitors. Introduction of either electron-withdrawing or donating groups onto phenyl acetate resulted in reduction in their rate of hydrolysis by PON1.
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