Tavori_2011_Free.Radic.Biol.Med_50_148

Reference

Title : Human carotid lesion linoleic acid hydroperoxide inhibits paraoxonase 1 (PON1) activity via reaction with PON1 free sulfhydryl cysteine 284 - Tavori_2011_Free.Radic.Biol.Med_50_148
Author(s) : Tavori H , Aviram M , Khatib S , Musa R , Mannheim D , Karmeli R , Vaya J
Ref : Free Radic Biol Med , 50 :148 , 2011
Abstract :

Paraoxonase 1 (PON1) is an HDL-associated lactonase with antiatherogenic properties. These include dampening the oxidation properties of human carotid lesion lipid extract (LLE), which in turn inactivates the enzyme. The aims of this study were to identify the PON1 inhibitor in LLE and explore the mechanism of inhibition. LLE inhibited both recombinant PON1 and HDL-PON1 lactonase activity in a dose- and time-dependent manner. Addition of antioxidants or electrophiles to LLE did not prevent PON1 inhibition. LLE was unable to inhibit a PON1 mutant lacking Cys284, whereas it did inhibit all other PON1 mutants tested. The inhibitor in the LLE was identified as linoleic acid hydroperoxide (LA-OOH) and inhibition was specific to this hydroperoxide. During its inhibition, PON1 acted like a peroxidase enzyme, reducing LA-OOH to LA-hydroxide via its Cys284. A similar reaction occurred with external thiols, such as DDT or cysteine, which also prevented PON1 inhibition and restored enzyme activity after inhibition. Thus, the antiatherogenic properties of HDL could be, at least in part, related to the sulfhydryl-reducing characteristics of its associated PON1, which are further protected and recycled by the sulfhydryl amino acid cysteine.

PubMedSearch : Tavori_2011_Free.Radic.Biol.Med_50_148
PubMedID: 21044882

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Citations formats

Tavori H, Aviram M, Khatib S, Musa R, Mannheim D, Karmeli R, Vaya J (2011)
Human carotid lesion linoleic acid hydroperoxide inhibits paraoxonase 1 (PON1) activity via reaction with PON1 free sulfhydryl cysteine 284
Free Radic Biol Med 50 :148

Tavori H, Aviram M, Khatib S, Musa R, Mannheim D, Karmeli R, Vaya J (2011)
Free Radic Biol Med 50 :148