Novel Associations of Nonstructural Loci with Paraoxonase Activity

Author:

Quillen Ellen E.1,Rainwater David L.1,Dyer Thomas D.1,Carless Melanie A.1,Curran Joanne E.1,Johnson Matthew P.1,Göring Harald H. H.1,Cole Shelley A.1,Rutherford Sue1,MacCluer Jean W.1,Moses Eric K.1,Blangero John1,Almasy Laura1,Mahaney Michael C.1

Affiliation:

1. Department of Genetics, Texas Biomedical Research Institute, P.O. Box 760549, San Antonio, TX 78245-0549, USA

Abstract

The high-density-lipoprotein-(HDL-) associated esterase paraoxonase 1 (PON1) is a likely contributor to the antioxidant and antiatherosclerotic capabilities of HDL. Two nonsynonymous mutations in the structural gene,PON1, have been associated with variation in activity levels, but substantial interindividual differences remain unexplained and are greatest for substrates other than the eponymous paraoxon. PON1 activity levels were measured for three substrates—organophosphate paraoxon, arylester phenyl acetate, and lactone dihydrocoumarin—in 767 Mexican American individuals from San Antonio, Texas. Genetic influences on activity levels for each substrate were evaluated by association with approximately one million single nucleotide polymorphism (SNPs) while conditioning onPON1genotypes. Significant associations were detected at five loci including regions on chromosomes 4 and 17 known to be associated with atherosclerosis and lipoprotein regulation and loci on chromosome 3 that regulate ubiquitous transcription factors. These loci explain 7.8% of variation in PON1 activity with lactone as a substrate, 5.6% with the arylester, and 3.0% with paraoxon. In light of the potential importance ofPON1in preventing cardiovascular disease/events, these novel loci merit further investigation.

Funder

National Institutes of Health

Publisher

Hindawi Limited

Subject

Biochemistry

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