Literature DB >> 23963787

Complex multilocus effects of catechol-O-methyltransferase haplotypes predict pain and pain interference 6 weeks after motor vehicle collision.

Andrey V Bortsov1, Luda Diatchenko, Samuel A McLean.   

Abstract

Catechol-O-methyltransferase, encoded by COMT gene, is the primary enzyme that metabolizes catecholamines. COMT haplotypes have been associated with vulnerability to persistent non-traumatic pain. In this prospective observational study, we investigated the influence of COMT on persistent pain and pain interference with life functions after motor vehicle collision (MVC) in 859 European American adults for whom overall pain (0-10 numeric rating scale) and pain interference (Brief Pain Inventory) were assessed at week 6 after MVC. Ten single nucleotide polymorphisms spanning the COMT gene were successfully genotyped, and nine were present in three haploblocks: block 1 (rs2020917, rs737865, rs1544325), block 2 (rs4633, rs4818, rs4680, rs165774), and block 3 (rs174697, rs165599). After adjustment for multiple comparisons, haplotype TCG from block 1 predicted decreased pain interference (p = 0.004). The pain-protective effect of the low pain sensitivity (CGGG) haplotype from block 2 was only observed if at least one TCG haplotype was present in block 1 (haplotype × haplotype interaction p = 0.002 and <0.0001 for pain and pain interference, respectively). Haplotype AG from block 3 was associated with pain and interference in males only (sex × haplotype interaction p = 0.005 and 0.0005, respectively). These results suggest that genetic variants in the distal promoter are important contributors to the development of persistent pain after MVC, directly and via the interaction with haplotypes in the coding region of the gene.

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Year:  2013        PMID: 23963787      PMCID: PMC3946256          DOI: 10.1007/s12017-013-8255-9

Source DB:  PubMed          Journal:  Neuromolecular Med        ISSN: 1535-1084            Impact factor:   3.843


  48 in total

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Authors:  L M Jacobsen; E I Schistad; A Storesund; L M Pedersen; L J Rygh; C Røe; J Gjerstad
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2.  A highly significant association between a COMT haplotype and schizophrenia.

Authors:  Sagiv Shifman; Michal Bronstein; Meira Sternfeld; Anne Pisanté-Shalom; Efrat Lev-Lehman; Avraham Weizman; Ilya Reznik; Baruch Spivak; Nimrod Grisaru; Leon Karp; Richard Schiffer; Moshe Kotler; Rael D Strous; Marnina Swartz-Vanetik; Haim Y Knobler; Eilat Shinar; Jacques S Beckmann; Benjamin Yakir; Neil Risch; Naomi B Zak; Ariel Darvasi
Journal:  Am J Hum Genet       Date:  2002-10-25       Impact factor: 11.025

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4.  Genetic variation in the beta2-adrenergic receptor but not catecholamine-O-methyltransferase predisposes to chronic pain: results from the 1958 British Birth Cohort Study.

Authors:  Lynne J Hocking; Blair H Smith; Gareth T Jones; David M Reid; David P Strachan; Gary J Macfarlane
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5.  Significance of catechol-O-methyltransferase gene polymorphism in fibromyalgia syndrome.

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7.  Haplotype associations with quantitative traits in the presence of complex multilocus and heterogeneous effects.

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Journal:  Genet Epidemiol       Date:  2009-01       Impact factor: 2.135

8.  The relationship between a common catechol-O-methyltransferase (COMT) polymorphism val(158) met and fibromyalgia.

Authors:  H Cohen; L Neumann; Y Glazer; R P Ebstein; D Buskila
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9.  Catechol-O-methyltransferase inhibition increases pain sensitivity through activation of both beta2- and beta3-adrenergic receptors.

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10.  The catechol-O-methyltransferase gene (COMT) and cognitive function from childhood through adolescence.

Authors:  Darya Gaysina; Man K Xu; Jennifer H Barnett; Tim J Croudace; Andrew Wong; Marcus Richards; Peter B Jones
Journal:  Biol Psychol       Date:  2012-11-21       Impact factor: 3.251

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  19 in total

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Authors:  Timothy F Platts-Mills; Sean A Flannigan; Andrey V Bortsov; Samantha Smith; Robert M Domeier; Robert A Swor; Phyllis L Hendry; David A Peak; Niels K Rathlev; Jeffrey S Jones; David C Lee; Francis J Keefe; Philip D Sloane; Samuel A McLean
Journal:  Ann Emerg Med       Date:  2015-06-16       Impact factor: 5.721

2.  Associations Between Catecholaminergic and Serotonergic Genes and Persistent Arm Pain Severity Following Breast Cancer Surgery.

Authors:  Mitchell R Knisely; Yvette P Conley; Betty Smoot; Steven M Paul; Jon D Levine; Christine Miaskowski
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4.  Advancements in Imaging Technology: Do They (or Will They) Equate to Advancements in Our Knowledge of Recovery in Whiplash?

Authors:  James M Elliott; Sudarshan Dayanidhi; Charles Hazle; Mark A Hoggarth; Jacob McPherson; Cheryl L Sparks; Kenneth A Weber
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5.  Whiplash-Associated Dysphagia: Considerations of Potential Incidence and Mechanisms.

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6.  Pain, Genes, and Function in the Post-Hip Fracture Period.

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7.  Association of Epidemiologic Factors and Genetic Variants Influencing Hypothalamic-Pituitary-Adrenocortical Axis Function With Postconcussive Symptoms After Minor Motor Vehicle Collision.

Authors:  Lauriane Auvergne; Andrey V Bortsov; Jacob C Ulirsch; David A Peak; Jeffrey S Jones; Robert A Swor; Robert M Domeier; David C Lee; Niels K Rathlev; Phyllis L Hendry; Samuel A McLean
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Review 8.  Individual differences in pain: understanding the mosaic that makes pain personal.

Authors:  Roger B Fillingim
Journal:  Pain       Date:  2017-04       Impact factor: 7.926

9.  Modification of COMT-dependent pain sensitivity by psychological stress and sex.

Authors:  Carolina B Meloto; Andrey V Bortsov; Eric Bair; Erika Helgeson; Cara Ostrom; Shad B Smith; Ronald Dubner; Gary D Slade; Roger B Fillingim; Joel D Greenspan; Richard Ohrbach; William Maixner; Samuel A McLean; Luda Diatchenko
Journal:  Pain       Date:  2016-04       Impact factor: 7.926

10.  CRHBP polymorphisms predict chronic pain development following motor vehicle collision.

Authors:  Sarah D Linnstaedt; Andrey V Bortsov; April C Soward; Robert Swor; David A Peak; Jeffrey Jones; Niels Rathlev; David C Lee; Robert Domeier; Phyllis L Hendry; Samuel A McLean
Journal:  Pain       Date:  2016-01       Impact factor: 7.926

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