Literature DB >> 26573179

PON1 Q192R genetic variant and response to clopidogrel and prasugrel: pharmacokinetics, pharmacodynamics, and a meta-analysis of clinical outcomes.

Jessica L Mega1, Sandra L Close2, Stephen D Wiviott3, Michael Man4, Suman Duvvuru4, Joseph R Walker5, Scott S Sundseth6, Jean-Philippe Collet7, Jessica T Delaney8, Jean-Sebastien Hulot9,10, Sabina A Murphy3, Guillaume Paré11, Matthew J Price12, Dirk Sibbing13, Tabassome Simon14, Dietmar Trenk15, Elliott M Antman3, Marc S Sabatine16.   

Abstract

Clopidogrel and prasugrel are antiplatelet therapies commonly used to treat patients with cardiovascular disease. They are both pro-drugs requiring biotransformation into active metabolites. It has been proposed that a genetic variant Q192R (rs662 A>G) in PON1 significantly alters the biotransformation of clopidogrel and affects clinical outcomes; however, this assertion has limited support. The relationship between this variant and clinical outcomes with prasugrel has not been studied. We genotyped PON1 Q192R in 275 healthy subjects treated with clopidogrel or prasugrel and 2922 patients with an ACS undergoing PCI randomized to treatment with clopidogrel or prasugrel in the TRITON-TIMI 38 trial. A meta-analysis was performed including 13 studies and 16,760 clopidogrel-treated patients. Among clopidogrel-treated subjects, there were no associations between Q192R and active drug metabolite levels (P = 0.62) or change in platelet aggregation (P = 0.51). Consistent with these results, in clopidogrel-treated patients in TRITON-TIMI 38, there was no association between Q192R and the rates of CV death, myocardial infarction, or stroke (RR 11.2 %, QR 8.6 %, and QQ 9.3 %; P = 0.66) or stent thrombosis (RR 2.4 %, QR 0.7 %, and QQ 1.6 %, P = 0.30), with patients with the putative at-risk Q variant having numerically lower event rates. Likewise, among prasugrel-treated subjects, there were no associations between Q192R and active drug metabolite levels (P = 0.88), change in platelet aggregation (P = 0.97), or clinical outcomes (P = 0.72). In a meta-analysis, the Q variant was not significantly associated with MACE (QQ vs. RR 1.22, 95 % CI 0.84-1.76) or stent thrombosis (QQ vs. RR OR 1.36, 95 % CI 0.77-2.38). Furthermore, when restricted to the validation studies, the OR (95 % CI) for MACE and stent thrombosis were 0.99 (0.77-1.27) and 1.23 (0.74-2.03), respectively. In the present study, the Q192R genetic variant in PON1 was not associated with the pharmacologic or clinical response to clopidogrel, nor was it associated with the response to prasugrel. The meta-analysis reinforced a lack of a significant association between Q192R and cardiovascular outcomes in clopidogrel-treated patients.

Entities:  

Keywords:  Clopidogrel; Genetics; PON1; Prasugrel

Mesh:

Substances:

Year:  2016        PMID: 26573179     DOI: 10.1007/s11239-015-1264-9

Source DB:  PubMed          Journal:  J Thromb Thrombolysis        ISSN: 0929-5305            Impact factor:   2.300


  33 in total

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2.  Paraoxonase-1 Q192R polymorphism and antiplatelet effects of clopidogrel in patients undergoing elective coronary stent placement.

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Journal:  JAMA       Date:  2011-10-26       Impact factor: 56.272

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Authors:  Alan R Shuldiner; Jeffrey R O'Connell; Kevin P Bliden; Amish Gandhi; Kathleen Ryan; Richard B Horenstein; Coleen M Damcott; Ruth Pakyz; Udaya S Tantry; Quince Gibson; Toni I Pollin; Wendy Post; Afshin Parsa; Braxton D Mitchell; Nauder Faraday; William Herzog; Paul A Gurbel
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8.  Intensive oral antiplatelet therapy for reduction of ischaemic events including stent thrombosis in patients with acute coronary syndromes treated with percutaneous coronary intervention and stenting in the TRITON-TIMI 38 trial: a subanalysis of a randomised trial.

Authors:  Stephen D Wiviott; Eugene Braunwald; Carolyn H McCabe; Ivan Horvath; Matyas Keltai; Jean-Paul R Herrman; Frans Van de Werf; William E Downey; Benjamin M Scirica; Sabina A Murphy; Elliott M Antman
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9.  Paraoxonase-1 is not a major determinant of stent thrombosis in a Taiwanese population.

Authors:  Dong-Yi Chen; Chao-Yung Wang; Ming-Shien Wen; Tsong-Hai Lee; Yen Chu; Ming-Jer Hsieh; Shang-Hung Chang; Cheng-Hung Lee; Jian-Liang Wang; Chun-Chi Chen; Laing-Suei Lu; Ming-Ta Lee; San-Jou Yeh; Fun-Chiung Lin; I-Chang Hsieh
Journal:  PLoS One       Date:  2012-06-18       Impact factor: 3.240

Review 10.  The association of the PON1 Q192R polymorphism with coronary heart disease: findings from the British Women's Heart and Health cohort study and a meta-analysis.

Authors:  Debbie A Lawlor; Ian N M Day; Tom R Gaunt; Lesley J Hinks; Patricia J Briggs; Matthew Kiessling; Nick Timpson; George Davey Smith; Shah Ebrahim
Journal:  BMC Genet       Date:  2004-06-23       Impact factor: 2.797
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3.  Effects of PON1 Gene Promoter DNA Methylation and Genetic Variations on the Clinical Outcomes of Dual Antiplatelet Therapy for Patients Undergoing Percutaneous Coronary Intervention.

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6.  Pharmacogenetic association study on clopidogrel response in Puerto Rican Hispanics with cardiovascular disease: a novel characterization of a Caribbean population.

Authors:  Dagmar F Hernandez-Suarez; Mariana R Botton; Stuart A Scott; Matthew I Tomey; Mario J Garcia; Jose Wiley; Pedro A Villablanca; Kyle Melin; Angel Lopez-Candales; Jessicca Y Renta; Jorge Duconge
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Review 7.  Paraoxonase (PON)-1: a brief overview on genetics, structure, polymorphisms and clinical relevance.

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8.  Association of PON1 gene promoter DNA methylation with the risk of Clopidogrel resistance in patients with coronary artery disease.

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Journal:  J Clin Lab Anal       Date:  2019-03-19       Impact factor: 2.352

9.  Impact of selected genetic factors on clopidogrel inactive metabolite level and antiplatelet response in patients after percutaneous coronary intervention.

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10.  Evaluation of the effect of carrier material on modification of release characteristics of poor water soluble drug from liquisolid compacts.

Authors:  Beenish Ali; Amjad Khan; Hamad S Alyami; Majeed Ullah; Abdul Wahab; Munair Badshah; Attiqa Naz
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