Do genetic predictors of pain sensitivity associate with persistent widespread pain?

doi:10.1186/1744-8069-5-56

Molecular Pain

Volume 5

Viewing options:

Abstract
Full text
PDF (421KB)

Associated material:

Related literature:

Articles citing this article
on Google Scholar
on ISI Web of Science
on PubMed Central
Other articles by authors
on Google Scholar

Holliday KL
Nicholl BI
Macfarlane GJ
Thomson W
Davies KA
McBeth J

on PubMed

Holliday KL
Nicholl BI
Macfarlane GJ
Thomson W
Davies KA
McBeth J
Related articles/pages
on Google

on Google Scholar

on PubMed

Tools:

Post to:

Short report

Do genetic predictors of pain sensitivity associate with persistent widespread pain?

Kate L Holliday ¹^* , Barbara I Nicholl¹^* , Gary J Macfarlane² , Wendy Thomson¹ , Kelly A Davies¹ and John McBeth¹

¹Arthritis Research Campaign Epidemiology Unit, University of Manchester, Manchester, UK

²Aberdeen Pain Research Collaboration (Epidemiology Group), School of Medicine and Dentistry, University of Aberdeen, Aberdeen, UK

author email corresponding author email* Contributed equally

Molecular Pain 2009, 5:56doi:10.1186/1744-8069-5-56


Published:	23 September 2009

Abstract

Genetic risk factors for pain sensitivity may also play a role in susceptibility to chronic pain disorders, in which subjects have low pain thresholds. The aim of this study was to determine if proposed functional single nucleotide polymorphisms (SNPs) in the GTP cyclohydrolase (GCH1) and μ opioid receptor (OPRM1) genes previously associated with pain sensitivity affect susceptibility to chronic widespread pain (CWP). Pain data was collected using body manikins via questionnaire at three time-points over a four year period from subjects aged 25-65 in the North-West of England as part of a population based cohort study, EPIFUND. CWP was defined at each time point using standard criteria. Three SNPs forming a proposed "pain-protective" haplotype in GCH1 (rs10483639, rs3783641 and rs8007267) and two SNPs in OPRM1 (rs1777971 (A118G) and rs563649) were genotyped in cases with persistent CWP (CWP present at ≥2 time-points) and controls who were pain-free at all time-points. The expectation-maximisation algorithm was used to estimate haplotype frequencies. The frequency of the "pain-protective" (CAT - C allele of rs10483639, A allele of rs3783641 and T allele of rs8007267) haplotype was compared to the frequency of the other haplotypes between cases and controls using the χ²test. Allele frequencies and carriage of the minor allele was compared between cases and controls using χ²tests for the OPRM1 SNPs. The frequency of the proposed GCH1 "pain-protective" haplotype (CAT) did not significantly differ between cases and controls and no significant associations were observed between the OPRM1 SNPs and CWP. In conclusion, there was no evidence of association between proposed functional SNPs, previously reported to influence pain sensitivity, in GCH1 and OPRM1 with CWP. Further evidence of null association in large independent cohorts is required to truly exclude these SNPs as genetic risk factors for CWP.