Evidence for a biopsychosocial influence on shoulder pain: Pain catastrophizing and catechol- O -methyltransferase (COMT) diplotype predict clinical pain ratings

George, Steven Z.; Wallace, Margaret R.; Wright, Thomas W.; Moser, Michael W.; Greenfield, Warren H.; Sack, Brandon K.; Herbstman, Deborah M.; Fillingim, Roger B.

doi:10.1016/j.pain.2007.06.019

Cited by 151 publications

(135 citation statements)

References 49 publications

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“…47 We considered COMT genotype in this study because of its high-priority candidate rating 11 and its previous influence on pain perception for healthy participants, 13-15 and also those seeking surgical treatment for shoulder pain. 2 We did not detect a main effect for COMT genotype in the current study, however, our primary hypothesis did not involve testing main effects of COMT genotype. We were most interested in investigating whether an interaction between pain catastrophizing and COMT diplotype had the potential to influence reports of induced shoulder pain.…”

Section: Discussionmentioning

confidence: 69%

Biopsychosocial Influence on Exercise-induced Delayed Onset Muscle Soreness at the Shoulder: Pain Catastrophizing and Catechol-O-Methyltransferase (COMT) Diplotype Predict Pain Ratings

George

Dover²,

Wallace

et al. 2008

The Clinical Journal of Pain

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Objective-The experience of pain is believed to be influenced by psychologic and genetic factors. A previous study suggested pain catastrophizing and catechol-O-methyltransferase (COMT) genotype influenced clinical pain ratings for patients seeking operative treatment of shoulder pain. This study investigated whether these same psychologic and genetic factors predicted responses to induced shoulder pain.Methods-Participants (n=63) completed self-report questionnaires and had COMT genotype determined before performing a standardized fatigue protocol to induce delayed onset muscle soreness. Then, shoulder pain ratings, self-report of upper-extremity disability ratings, and muscle torque production were reassessed 24, 48, and 72 hours later.Results-This cohort consisted of 35 women and 28 men, with a mean age of 20.9 years (SD=1.7). The frequency of COMT diplotypes was 42 with "high COMT enzyme activity" (low pain sensitivity group) and 21 with "low COMT enzyme activity" (average pain sensitivity/high pain sensitivity group). A hierarchical regression model indicated that an interaction between pain catastrophizing and COMT diplotype was the strongest unique predictor of 72-hour pain ratings. The same interaction was not predictive of self-report of disability or muscle torque production at 72 hours. The pain catastrophizing × COMT diplotype interaction indicated that participants with high pain catastrophizing and low COMT enzyme activity (average pain sensitivity/high pain sensitivity group) were more likely (relative risk=3.5, P=0.025) to have elevated pain intensity ratings (40/100 or higher).Reprints: Steven Z. George, PT, PhD, Department of Physical Therapy, Brooks Center for Rehabilitation Studies, University of Florida, Health Science Center, PO Box 100154, Gainesville, FL 32610-0154 (e-mail: E-mail: szgeorge@phhp.ufl.edu). NIH Public Access Author ManuscriptClin J Pain. Author manuscript; available in PMC 2009 April 16. NIH-PA Author ManuscriptNIH-PA Author Manuscript NIH-PA Author ManuscriptDiscussion-These findings from an experimental model converge with those from a surgical cohort and provide additional evidence that the presence of elevated pain catastrophizing and COMT diplotype indicative of low COMT enzyme activity have the potential to increase the risk of developing chronic pain syndromes.Keywords biopsychosocial model; chronic pain; catastrophizing; COMT genotype; shoulder pain; delayed onset muscle sorenessThe experience of pain varies considerably among individuals. Social, cultural, environmental, psychologic, and genetic factors are all believed to contribute to this variability. A model for the development of idiopathic pain conditions that takes into consideration these sources of variability was recently proposed. 1 In this model, it is suggested that high levels of psychologic distress and pain amplification (ie, genetic predisposition for biologic or physiologic processes) are the primary factors contributing to the development of idiopathic pain conditions. 1Few studies to da...

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Section: Discussionmentioning

confidence: 69%

Biopsychosocial Influence on Exercise-induced Delayed Onset Muscle Soreness at the Shoulder: Pain Catastrophizing and Catechol-O-Methyltransferase (COMT) Diplotype Predict Pain Ratings

George

Dover²,

Wallace

et al. 2008

The Clinical Journal of Pain

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“…Empirically, catastrophising is identified by heightened perception of pain (Finan et al, 2011;George et al, 2008;Edwards, 2006). The next question is whether catastrophising is caused by the same genetic factors as pain perception, or rather, if it acts on those genes to modify their influence on pain.…”

Section: Genetics Of Variability In Psychosocial Phenotypesmentioning

confidence: 99%

Molecular Genetics of Variability in Human Pain

Belfer

Shnol

Finelli

2013

Encyclopedia of Life Sciences

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Pain is considered to be an evolutionary‐conserved trait and is employed as a necessary means to survival. Although this trait is common in all humans, it shows great variability among individuals. The underlying mechanisms of pain perception are not fully understood. Functional single nucleotide polymorphism and other types of genetic polymorphisms increase or decrease gene function influencing the encoded product. These polymorphisms (alleles) used to analyse the genetic mechanisms of pain perception may account for up to 50% of the total variability in the human pain phenotype. Interestingly, certain genes (e.g. COMT and OPRM1 ) are reoccurring targets of interest for the variation they cause in experimental and clinical pain perception as well for their effects on analgesia and pain‐related psychosocial traits. Current and future genetic studies of human pain will reveal missing risk factors for painful disorders and will aid focussed clinical trials for improved and innovative pain management in patients at risk. Key Concepts: Variability is a common feature for all pain phenotypes in humans. Genetics account for a big portion of overall variability in human pain. Different pain phenotypes have overlapping genetic background. Both common and rare functional genetic polymorphisms contribute to human pain. Candidate gene studies revealed only of a handful of genetic risk and protective factors for human pain. Unbiased genome‐wide approaches will provide data on additional genetic factors influencing human pain.

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“…39,[53][54][55] As in the management of patients with low back pain, 24,27 there are ongoing efforts to improve diagnostic 35,42 and prognostic 28,29 approaches to managing patients with shoulder disorders. Currently there is an abundance of special tests and measures used to investigate shoulder pain.…”

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“…29 Participants provided informed consent, in keeping with guidelines set forth by The University of tions. 9,32,38,44 Local PPT was defined as the average of the 3 shoulder measures (supraspinatus, infraspinatus, and acromion process), and distal PPT was defined as the average of the 2 nonshoulder measures (brachioradialis and masseter).…”

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confidence: 99%

Thermal and Pressure Pain Sensitivity in Patients with Unilateral Shoulder Pain: Comparison of Involved and Uninvolved Sides

Coronado¹,

Kindler²,

Valencia³

et al. 2011

J Orthop Sports Phys Ther

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Evidence for a biopsychosocial influence on shoulder pain: Pain catastrophizing and catechol- O -methyltransferase (COMT) diplotype predict clinical pain ratings

Cited by 151 publications

References 49 publications

Biopsychosocial Influence on Exercise-induced Delayed Onset Muscle Soreness at the Shoulder: Pain Catastrophizing and Catechol-O-Methyltransferase (COMT) Diplotype Predict Pain Ratings

Biopsychosocial Influence on Exercise-induced Delayed Onset Muscle Soreness at the Shoulder: Pain Catastrophizing and Catechol-O-Methyltransferase (COMT) Diplotype Predict Pain Ratings

Molecular Genetics of Variability in Human Pain

Thermal and Pressure Pain Sensitivity in Patients with Unilateral Shoulder Pain: Comparison of Involved and Uninvolved Sides

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