Paraoxonase (PON1) Phenotype Is a Better Predictor of Vascular Disease Than Is
 PON1
 192
 or
 PON1
 55
 Genotype

Jarvik, Gail P.; Rozek, Laura S.; Brophy, Victoria H.; Hatsukami, Thomas S.; Richter, Rebecca J.; Schellenberg, Gerard D.; Furlong, Clement E.

doi:10.1161/01.atv.20.11.2441

Cited by 293 publications

(241 citation statements)

References 46 publications

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“…Thus, it is likely that paraoxon and phenylacetate seemed to be better surrogate substrates than diazoxon for measuring PON1 activity. Jarvik et al (2000) found that the PON1 activity towards diazoxon was more predictive of vascular disease status than was the PON1 activity towards paraoxon in marginal analysis. However, in the only prospective study published so far, paraoxon but not diazoxon hydrolysis was an independent risk factor for CHD events (Mackness et al 2003).…”

Section: Discussionmentioning

confidence: 93%

Paraoxonase 1 status in the Thai population

et al. 2005

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Human serum paraoxonase 1 (PON1), a highdensity lipoprotein (HDL)-associated enzyme, has been shown to reduce the oxidation of low-density lipoprotein (LDL) and HDL by degrading lipid peroxides. This property of PON1 accounts for its ability to protect against atherosclerosis. In this study, we identified four polymorphisms in both the coding (L55M and Q192R) and regulatory regions (T-108C and G-909C) of the human PON1 gene in 202 healthy Thai individuals and investigated the influence of these polymorphisms on serum PON1 activity towards three substrates, namely, paraoxon, phenylacetate and diazoxon. The PON1 L55M, Q192R and G-909C polymorphisms significantly affected the variation in serum PON1 activity towards paraoxon. Serum PON1 activity towards paraoxon was significantly different among the genotype groups, as follows: 55LL > 55LM/55MM, 192RR > 192QR > 192QQ and À909CC > À909CG > À909GG. The PON1 Q192R and G-909C polymorphisms also influenced the variation in serum PON1 activity towards diazoxon but in the opposite direction to the activity towards paraoxon. Only the PON1 L55M polymorphism was associated with significant variation in serum PON1 activity towards phenylacetate while the PON1 T-108C polymorphism had no significant effect on serum PON1 activity towards any substrate. We also found linkage disequilibrium among the polymorphic sites, including Q192R versus L55M, Q192R versus T-108C and Q192R versus G-909C. Serum PON1 activity towards both paraoxon and phenylacetate, but not diazoxon, was positively correlated with HDL cholesterol (HDL-C) and apo AI concentrations. None of the PON1 polymorphisms significantly affected serum lipid, lipoprotein or apolipoprotein concentrations. Our findings suggest that the physiological relevance of the PON1 polymorphisms is that they are associated with significant differences in serum PON1 activity, and the impact of PON1 polymorphisms on this activity is substrate-dependent.

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Section: Discussionmentioning

confidence: 93%

Paraoxonase 1 status in the Thai population

et al. 2005

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“…These standards showed less than 8% variability between independent assays. An additional 26 samples from a previously determined PON1 status frequency distribution of known phenotypes and genotypes (Jarvik et al, 2000) were included as additional standards for CPOase assays. There was a mean 4.4% variation between assays for these 29 samples.…”

Section: Pon1 Inferred Genotype and Chlorpyrifosoxonase Activitymentioning

confidence: 99%

Paraoxonase status and plasma butyrylcholinesterase activity in chlorpyrifos manufacturing workers

Albers

Garabrant

Berent

et al. 2009

J Expo Sci Environ Epidemiol

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Chlorpyrifos is an organophosphorus (OP) anticholinesterase insecticide. Paraoxonase (PON1) is an enzyme found in liver and plasma that hydrolyzes a number of OP compounds. PON1 polymorphisms include a glutamine (Q)/arginine (R) substitution at position 192 (PON1 Q192R ) that affects hydrolysis of OP substrates, with the PON1 192Q allotype hydrolyzing chlorpyrifos oxon less efficiently than the PON1 192R allotype, a variation potentially important in determining susceptibility to chlorpyrifos. We studied 53 chlorpyrifos workers and 60 referents during 1 year and estimated chlorpyrifos exposure using industrial hygiene and employment records and excretion of the chlorpyrifos metabolite 3,5,6-trichloro-2-pyridinol (TCP). Plasma butyrylcholinesterase (BuChE) activity, which may by inhibited by chlorpyrifos exposure, was measured monthly. In addition, plasma samples were assayed for paraoxonase (PONase), diazoxonase (DZOase), and chlorpyrifosoxonase (CPOase) activity to determine PON1 status (inferred genotypes and their functional activity). Linear regression analyses modeled BuChE activity as a function of chlorpyrifos exposure and covariates. We postulated that the level of CPOase activity and the inferred PON1 192 genotype (together reflecting PON1 status) would differ between groups and that PON1 status would modify the models of chlorpyrifos exposure on BuChE activity. Chlorpyrifos workers and referents had a 100-fold difference in cumulative chlorpyrifos exposure. Contrary to our hypotheses, mean CPOase activity was similar in both groups (P ¼ 0.58) and PON1 192Q showed a slight overrepresentation, not an underrepresentation, in the chlorpyrifos group compared with referents (PON1 192QQ , 51% chlorpyrifos, 40% referent; PON 192QR , 43% chlorpyrifos, 40% referent; PON 192RR , 6% chlorpyrifos, 20% referent, P ¼ 0.08). In our models, BuChE activity was significantly inversely associated with measures of interim chlorpyrifos exposure, but the biological effects of chlorpyrifos exposure on BuChE activity were not modified by PON1 inferred genotype or CPOase activity.

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“…57,58 Unfortunately, paraoxonase activity is calcium dependent and cannot be measured in the plateletrich plasma we have collected from our entire sample. We have thus begun assessing paraoxonase, diazoxonase, and arylesterase activity in all 217 serum samples currently available from the AGRE collection, 30 including 40 families with one or more autistic patients and their first-degree relatives.…”

Section: Markersmentioning

confidence: 99%

Paraoxonase gene variants are associated with autism in North America, but not in Italy: possible regional specificity in gene–environment interactions

et al. 2005

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Organophosphates (OPs) are routinely used as pesticides in agriculture and as insecticides within the household. Our prior work on Reelin and APOE delineated a gene-environment interactive model of autism pathogenesis, whereby genetically vulnerable individuals prenatally exposed to OPs during critical periods in neurodevelopment could undergo altered neuronal migration, resulting in an autistic syndrome. Since household use of OPs is far greater in the USA than in Italy, this model was predicted to hold validity in North America, but not in Europe. Here, we indirectly test this hypothesis by assessing linkage/association between autism and variants of the paraoxonase gene (PON1) encoding paraoxonase, the enzyme responsible for OP detoxification. Three functional single nucleotide polymorphisms, PON1 CÀ108T, L55M, and Q192R, were assessed in 177 Italian and 107 Caucasian-American complete trios with primary autistic probands. As predicted, Caucasian-American and not Italian families display a significant association between autism and PON1 variants less active in vitro on the OP diazinon (R192), according to case-control contrasts (Q192R: v 2 ¼ 6.33, 1 df, Po0.025), transmission/disequilibrium tests (Q192R: TDT v 2 ¼ 5.26, 1 df, Po0.025), familybased association tests (Q192R and L55M: FBAT Z ¼ 2.291 and 2.435 respectively, Po0.025), and haplotype-based association tests (L55/R192: HBAT Z ¼ 2.430, Po0.025). These results are consistent with our model and provide further support for the hypothesis that concurrent genetic vulnerability and environmental OP exposure may possibly contribute to autism pathogenesis in a sizable subgroup of North American individuals.

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Paraoxonase (PON1) Phenotype Is a Better Predictor of Vascular Disease Than Is PON1 ₁₉₂ or PON1 ₅₅ Genotype

Cited by 293 publications

References 46 publications

Paraoxonase 1 status in the Thai population

Paraoxonase 1 status in the Thai population

Paraoxonase status and plasma butyrylcholinesterase activity in chlorpyrifos manufacturing workers

Paraoxonase gene variants are associated with autism in North America, but not in Italy: possible regional specificity in gene–environment interactions

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Paraoxonase (PON1) Phenotype Is a Better Predictor of Vascular Disease Than Is PON1 192 or PON1 55 Genotype

Cited by 293 publications

References 46 publications

Paraoxonase 1 status in the Thai population

Paraoxonase 1 status in the Thai population

Paraoxonase status and plasma butyrylcholinesterase activity in chlorpyrifos manufacturing workers

Paraoxonase gene variants are associated with autism in North America, but not in Italy: possible regional specificity in gene–environment interactions

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Product

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Paraoxonase (PON1) Phenotype Is a Better Predictor of Vascular Disease Than Is PON1 ₁₉₂ or PON1 ₅₅ Genotype