OBJECTIVES: The aim of this study was to investigate the association between the catechol-O-methyltransferase (COMT) 'pain sensitivity' haplotypes and chronic widespread pain (CWP) in two distinct cohorts. METHODS: Cases of CWP and controls free of pain were selected from two population-based studies: the Epidemiology of Functional Disorders study (EPIFUND) (UK) and the European Male Ageing Study (European). The number of cases and controls were 164 and 172, and 204 and 935, respectively. Identical American College of Rheumatology criteria were used in both studies to ascertain CWP status. The EPIFUND study had three time points and cases were classified as subjects with CWP at two or three time points and controls as those free of pain at all three time points. Four single nucleotide polymorphisms (SNP): rs6269, rs4633, rs4818 and rs4680 (V158M) were genotyped using Sequenom technology. Allele and genotype frequencies were compared and haplotype analysis was conducted using PLINK software. RESULTS: No differences in allele or genotype frequencies for any of the four SNP were observed between cases and controls for either cohort. Haplotype analysis also showed no difference in the frequency of haplotypes between cases and controls. CONCLUSIONS: There was no evidence of association between the COMT 'pain sensitivity' haplotypes and CWP in two population-based cohorts.
OBJECTIVES: The aim of this study was to investigate the association between the catechol-O-methyltransferase (COMT) 'pain sensitivity' haplotypes and chronic widespread pain (CWP) in two distinct cohorts. METHODS: Cases of CWP and controls free of pain were selected from two population-based studies: the Epidemiology of Functional Disorders study (EPIFUND) (UK) and the European Male Ageing Study (European). The number of cases and controls were 164 and 172, and 204 and 935, respectively. Identical American College of Rheumatology criteria were used in both studies to ascertain CWP status. The EPIFUND study had three time points and cases were classified as subjects with CWP at two or three time points and controls as those free of pain at all three time points. Four single nucleotide polymorphisms (SNP): rs6269, rs4633, rs4818 and rs4680 (V158M) were genotyped using Sequenom technology. Allele and genotype frequencies were compared and haplotype analysis was conducted using PLINK software. RESULTS: No differences in allele or genotype frequencies for any of the four SNP were observed between cases and controls for either cohort. Haplotype analysis also showed no difference in the frequency of haplotypes between cases and controls. CONCLUSIONS: There was no evidence of association between the COMT 'pain sensitivity' haplotypes and CWP in two population-based cohorts.
Authors: Mitchell R Knisely; Yvette P Conley; Betty Smoot; Steven M Paul; Jon D Levine; Christine Miaskowski Journal: J Pain Date: 2019-03-21 Impact factor: 5.820
Authors: Lynn M Martire; Stephanie J Wilson; Brent J Small; Yvette P Conley; Piotr K Janicki; Martin J Sliwinski Journal: Scand J Pain Date: 2016-01-01
Authors: Marjolein J Peters; Linda Broer; Hanneke L D M Willemen; Gudny Eiriksdottir; Lynne J Hocking; Kate L Holliday; Michael A Horan; Ingrid Meulenbelt; Tuhina Neogi; Maria Popham; Carsten O Schmidt; Anushka Soni; Ana M Valdes; Najaf Amin; Elaine M Dennison; Niels Eijkelkamp; Tamara B Harris; Deborah J Hart; Albert Hofman; Frank J P M Huygen; Karen A Jameson; Gareth T Jones; Lenore J Launer; Hanneke J M Kerkhof; Marjolein de Kruijf; John McBeth; Margreet Kloppenburg; William E Ollier; Ben Oostra; Antony Payton; Fernando Rivadeneira; Blair H Smith; Albert V Smith; Lisette Stolk; Alexander Teumer; Wendy Thomson; André G Uitterlinden; Ke Wang; Sophie H van Wingerden; Nigel K Arden; Cyrus Cooper; David Felson; Vilmundur Gudnason; Gary J Macfarlane; Neil Pendleton; P Eline Slagboom; Tim D Spector; Henry Völzke; Annemieke Kavelaars; Cornelia M van Duijn; Frances M K Williams; Joyce B J van Meurs Journal: Ann Rheum Dis Date: 2012-09-06 Impact factor: 19.103