Literature DB >> 22074755

Potential genetic risk factors for chronic TMD: genetic associations from the OPPERA case control study.

Shad B Smith1, Dylan W Maixner, Joel D Greenspan, Ronald Dubner, Roger B Fillingim, Richard Ohrbach, Charles Knott, Gary D Slade, Eric Bair, Dustin G Gibson, Dmitri V Zaykin, Bruce S Weir, William Maixner, Luda Diatchenko.   

Abstract

UNLABELLED: Genetic factors play a role in the etiology of persistent pain conditions, putatively by modulating underlying processes such as nociceptive sensitivity, psychological well-being, inflammation, and autonomic response. However, to date, only a few genes have been associated with temporomandibular disorders (TMD). This study evaluated 358 genes involved in pain processes, comparing allelic frequencies between 166 cases with chronic TMD and 1,442 controls enrolled in the OPPERA (Orofacial Pain: Prospective Evaluation and Risk Assessment) study cooperative agreement. To enhance statistical power, 182 TMD cases and 170 controls from a similar study were included in the analysis. Genotyping was performed using the Pain Research Panel, an Affymetrix gene chip representing 3,295 single nucleotide polymorphisms, including ancestry-informative markers that were used to adjust for population stratification. Adjusted associations between genetic markers and TMD case status were evaluated using logistic regression. The OPPERA findings provided evidence supporting previously reported associations between TMD and 2 genes: HTR2A and COMT. Other genes were revealed as potential new genetic risk factors for TMD, including NR3C1, CAMK4, CHRM2, IFRD1, and GRK5. While these findings need to be replicated in independent cohorts, the genes potentially represent important markers of risk for TMD, and they identify potential targets for therapeutic intervention. PERSPECTIVE: Genetic risk factors for TMD pain were explored in the case-control component of the OPPERA cooperative agreement, a large population-based prospective cohort study. Over 350 candidate pain genes were assessed using a candidate gene panel, with several genes displaying preliminary evidence for association with TMD status. Published by Elsevier Inc.

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Year:  2011        PMID: 22074755      PMCID: PMC3268684          DOI: 10.1016/j.jpain.2011.08.005

Source DB:  PubMed          Journal:  J Pain        ISSN: 1526-5900            Impact factor:   5.820


  43 in total

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  52 in total

Review 1.  Summary of findings from the OPPERA baseline case-control study: implications and future directions.

Authors:  Roger B Fillingim; Gary D Slade; Luda Diatchenko; Ronald Dubner; Joel D Greenspan; Charles Knott; Richard Ohrbach; William Maixner
Journal:  J Pain       Date:  2011-11       Impact factor: 5.820

2.  Clinical findings and pain symptoms as potential risk factors for chronic TMD: descriptive data and empirically identified domains from the OPPERA case-control study.

Authors:  Richard Ohrbach; Roger B Fillingim; Flora Mulkey; Yoly Gonzalez; Sharon Gordon; Henry Gremillion; Pei-Feng Lim; Margarete Ribeiro-Dasilva; Joel D Greenspan; Charles Knott; William Maixner; Gary Slade
Journal:  J Pain       Date:  2011-11       Impact factor: 5.820

3.  Upregulation of fatty acid amide hydrolase in the dorsal periaqueductal gray is associated with neuropathic pain and reduced heart rate in rats.

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5.  Effect of Human Genetic Variability on Gene Expression in Dorsal Root Ganglia and Association with Pain Phenotypes.

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10.  The prevalence of comorbid symptoms of central sensitization syndrome among three different groups of temporomandibular disorder patients.

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