Seminars in Orthodontics
Volume 14, Issue 2 , Pages 146-156, June 2008

Orthodontic Treatment, Genetic Factors, and Risk of Temporomandibular Disorder

  • Gary D. Slade

      Affiliations

    • Professor of Oral Epidemiology, Dental School, University of Adelaide, Adelaide, Australia.
    • Corresponding Author InformationAddress correspondence to Gary D. Slade, BDSc, DDPH, PhD, Professor of Oral Epidemiology, Australian Research Centre for Population Oral Health, Dental School, University of Adelaide, SA 5005, Australia. Phone: +618-8303-3291; Fax: +618-8303-3070
  • ,
  • Luda Diatchenko

      Affiliations

    • Research Associate Professor, Center for Neurosensory Disorders, University of North Carolina, Chapel Hill, NC.
  • ,
  • Richard Ohrbach

      Affiliations

    • Associate Professor, Department of Oral Diagnostic Sciences, University at Buffalo, Buffalo, NY.
  • ,
  • William Maixner

      Affiliations

    • Professor, Center for Neurosensory Disorders, School of Dentistry, University of North Carolina, Chapel Hill, NC.

Traditionally, four groups of factors have been identified in the etiology of temporomandibular disorder (TMD): anatomical variation in the masticatory system; psychosocial characteristics; pain in other body regions; and demographics. Orthodontic treatment has been variously cited both as a protective and harmful factor in TMD etiology. Recently, a search has begun for a genetic influence on TMD etiology. Genetic markers can be of additional value in identifying gene-environment interactions, that is, isolating population subgroups, defined by genotype in which environmental influences play a relatively greater or lesser etiological role. This article reviews concepts and study design requirements for epidemiological investigations into TMD etiology. Findings are presented from a prospective cohort study of 186 females that illustrate an example of gene-environment interaction in TMD onset. Among people with a variant of the gene encoding catechol-O-methyltransferase, an enzyme associated with pain responsiveness, risk of developing TMD was significantly greater for subjects who reported a history of orthodontic treatment compared with subjects who did not (P = 0.04). While further studies are needed to investigate TMD etiology, this genetic variant potentially could help to identify patients whose risk of developing TMD is heightened following orthodontic treatment, hence serving as a risk marker useful in planning orthodontic care.

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 Supported by: NIH/NIDCR DE07509, NS045685, DE007333, AR/AI-44564, NIH Intramural Grants DE00366 and AA000301, and the Comprehensive Neuroscience Program Grant USUHS G192BR-C4

PII: S1073-8746(08)00011-X

doi:10.1053/j.sodo.2008.02.005

Seminars in Orthodontics
Volume 14, Issue 2 , Pages 146-156, June 2008