Literature DB >> 21878436

A genome-wide association study identifies a region at chromosome 12 as a potential susceptibility locus for restenosis after percutaneous coronary intervention.

M Lourdes Sampietro1, Stella Trompet, Jeffrey J W Verschuren, Rudolf P Talens, Joris Deelen, Bastiaan T Heijmans, Robbert J de Winter, Rene A Tio, Pieter A F M Doevendans, Santhi K Ganesh, Elizabeth G Nabel, Harm-Jan Westra, Lude Franke, Erik B van den Akker, Rudi G J Westendorp, Aeilko H Zwinderman, Adnan Kastrati, Werner Koch, P Eline Slagboom, Peter de Knijff, J Wouter Jukema.   

Abstract

Percutaneous coronary intervention (PCI) has become an effective therapy to treat obstructive coronary artery diseases (CAD). However, one of the major drawbacks of PCI is the occurrence of restenosis in 5-25% of all initially treated patients. Restenosis is defined as the re-narrowing of the lumen of the blood vessel, resulting in renewed symptoms and the need for repeated intervention. To identify genetic variants that are associated with restenosis, a genome-wide association study (GWAS) was conducted in 295 patients who developed restenosis (cases) and 571 who did not (controls) from the GENetic Determinants of Restenosis (GENDER) study. Analysis of ~550 000 single nucleotide polymorphisms (SNPs) in GENDER was followed by a replication phase in three independent case-control populations (533 cases and 3067 controls). A potential susceptibility locus for restenosis at chromosome 12, including rs10861032 (P(combined) = 1.11 × 10(-7)) and rs9804922 (P(combined) = 1.45 × 10(-6)), was identified in the GWAS and replication phase. In addition, both SNPs were also associated with coronary events (rs10861032, P(additive) = 0.005; rs9804922, P(additive) = 0.023) in a trial based cohort set of elderly patients with (enhanced risk of) CAD (PROSPER) and all-cause mortality in PROSPER (rs10861032, P(additive) = 0.007; rs9804922, P(additive) = 0.013) and GENDER (rs10861032, P(additive) = 0.005; rs9804922, P(additive) = 0.023). Further analysis suggests that this locus could be involved in regulatory functions.

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Year:  2011        PMID: 21878436      PMCID: PMC3209827          DOI: 10.1093/hmg/ddr389

Source DB:  PubMed          Journal:  Hum Mol Genet        ISSN: 0964-6906            Impact factor:   6.150


  56 in total

Review 1.  Genetic aspects of restenosis after percutaneous coronary interventions: towards more tailored therapy.

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3.  A meta-analysis of the angiotensin-converting enzyme gene polymorphism and restenosis after percutaneous transluminal coronary revascularization: evidence for publication bias.

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9.  Pravastatin in elderly individuals at risk of vascular disease (PROSPER): a randomised controlled trial.

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3.  Systematic testing of literature reported genetic variation associated with coronary restenosis: results of the GENDER Study.

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5.  Pathway analysis using genome-wide association study data for coronary restenosis--a potential role for the PARVB gene.

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6.  Non-homologous end-joining pathway associated with occurrence of myocardial infarction: gene set analysis of genome-wide association study data.

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Review 7.  Influence of the angiotensin converting enzyme insertion or deletion genetic variant and coronary restenosis risk: evidence based on 11,193 subjects.

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8.  Candidate Gene Analysis of Mortality in Dialysis Patients.

Authors:  Tonia C Rothuizen; Gurbey Ocak; Jeffrey J W Verschuren; Friedo W Dekker; Ton J Rabelink; J Wouter Jukema; Joris I Rotmans
Journal:  PLoS One       Date:  2015-11-20       Impact factor: 3.240

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