Literature DB >> 29185836

Exome-chip meta-analysis identifies association between variation in ANKRD26 and platelet aggregation.

Ming-Huei Chen1, Lisa R Yanek2, Joshua D Backman3, John D Eicher1, Jennifer E Huffman1, Yoav Ben-Shlomo4, Andrew D Beswick5, Laura M Yerges-Armstrong3, Alan R Shuldiner3, Jeffrey R O'Connell3, Rasika A Mathias6, Diane M Becker2, Lewis C Becker7, Joshua P Lewis3, Andrew D Johnson1, Nauder Faraday8.   

Abstract

Previous genome-wide association studies (GWAS) have identified several variants associated with platelet function phenotypes; however, the proportion of variance explained by the identified variants is mostly small. Rare coding variants, particularly those with high potential for impact on protein structure/function, may have substantial impact on phenotype but are difficult to detect by GWAS. The main purpose of this study was to identify low frequency or rare variants associated with platelet function using genotype data from the Illumina HumanExome Bead Chip. Three family-based cohorts of European ancestry, including ~4,000 total subjects, comprised the discovery cohort and two independent cohorts, one of European and one of African American ancestry, were used for replication. Optical aggregometry in platelet-rich plasma was performed in all the discovery cohorts in response to adenosine diphosphate (ADP), epinephrine, and collagen. Meta-analyses were performed using both gene-based and single nucleotide variant association methods. The gene-based meta-analysis identified a significant association (P = 7.13 × 10-7) between rare genetic variants in ANKRD26 and ADP-induced platelet aggregation. One of the ANKRD26 SNVs - rs191015656, encoding a threonine to isoleucine substitution predicted to alter protein structure/function, was replicated in Europeans. Aggregation increases of ~20-50% were observed in heterozygotes in all cohorts. Novel genetic signals in ABCG1 and HCP5 were also associated with platelet aggregation to ADP in meta-analyses, although only results for HCP5 could be replicated. The SNV in HCP5 intersects epigenetic signatures in CD41+ megakaryocytes suggesting a new functional role in platelet biology for HCP5. This is the first study to use gene-based association methods from SNV array genotypes to identify rare variants related to platelet function. The molecular mechanisms and pathophysiological relevance for the identified genetic associations requires further study.

Entities:  

Keywords:  Platelets; SNP; exome; genetic association; platelet aggregation; platelet reactivity

Mesh:

Substances:

Year:  2017        PMID: 29185836      PMCID: PMC6214797          DOI: 10.1080/09537104.2017.1384538

Source DB:  PubMed          Journal:  Platelets        ISSN: 0953-7104            Impact factor:   3.862


  33 in total

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Review 3.  Low-dose aspirin for the prevention of atherothrombosis.

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4.  Heritability of platelet function in families with premature coronary artery disease.

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Journal:  JAMA       Date:  2009-08-26       Impact factor: 56.272

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8.  Genome-wide meta-analyses identifies seven loci associated with platelet aggregation in response to agonists.

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Journal:  Nat Genet       Date:  2010-06-06       Impact factor: 38.330

9.  Mapping the platelet profile for functional genomic studies and demonstration of the effect size of the GP6 locus.

Authors:  C I Jones; S F Garner; W Angenent; A Bernard; C Berzuini; P Burns; R W Farndale; J Hogwood; A Rankin; J C Stephens; B D Tom; J Walton; F Dudbridge; W H Ouwehand; A H Goodall
Journal:  J Thromb Haemost       Date:  2007-08       Impact factor: 5.824

10.  HIV-1 disease-influencing effects associated with ZNRD1, HCP5 and HLA-C alleles are attributable mainly to either HLA-A10 or HLA-B*57 alleles.

Authors:  Gabriel Catano; Hemant Kulkarni; Weijing He; Vincent C Marconi; Brian K Agan; Michael Landrum; Stephanie Anderson; Judith Delmar; Vanessa Telles; Li Song; John Castiblanco; Robert A Clark; Matthew J Dolan; Sunil K Ahuja
Journal:  PLoS One       Date:  2008-11-04       Impact factor: 3.240

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2.  A large-scale exome array analysis of venous thromboembolism.

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Journal:  Genet Epidemiol       Date:  2019-01-19       Impact factor: 2.344

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4.  Cell-Specific PEAR1 Methylation Studies Reveal a Locus that Coordinates Expression of Multiple Genes.

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5.  G protein-coupled receptor kinase 5 regulates thrombin signaling in platelets via PAR-1.

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