Scholars@Duke publication: Whole-genome methylation profiling reveals regions associated with painful temporomandibular disorders and active recovery processes.

Whole-genome methylation profiling reveals regions associated with painful temporomandibular disorders and active recovery processes.

Publication , Journal Article

Ao, X; Parisien, M; Fillingim, RB; Ohrbach, R; Slade, GD; Diatchenko, L; Smith, SB

Published in: Pain

May 1, 2024

Temporomandibular disorders (TMDs), collectively representing one of the most common chronic pain conditions, have a substantial genetic component, but genetic variation alone has not fully explained the heritability of TMD risk. Reasoning that the unexplained heritability may be because of DNA methylation, an epigenetic phenomenon, we measured genome-wide DNA methylation using the Illumina MethylationEPIC platform with blood samples from participants in the Orofacial Pain: Prospective Evaluation and Risk Assessment (OPPERA) study. Associations with chronic TMD used methylation data from 496 chronic painful TMD cases and 452 TMD-free controls. Changes in methylation between enrollment and a 6-month follow-up visit were determined for a separate sample of 62 people with recent-onset painful TMD. More than 750,000 individual CpG sites were examined for association with chronic painful TMD. Six differentially methylated regions were significantly ( P < 5 × 10 -8 ) associated with chronic painful TMD, including loci near genes involved in the regulation of inflammatory and neuronal response. A majority of loci were similarly differentially methylated in acute TMD consistent with observed transience or persistence of symptoms at follow-up. Functional characterization of the identified regions found relationships between methylation at these loci and nearby genetic variation contributing to chronic painful TMD and with gene expression of proximal genes. These findings reveal epigenetic contributions to chronic painful TMD through methylation of the genes FMOD , PM20D1 , ZNF718 , ZFP57 , and RNF39 , following the development of acute painful TMD. Epigenetic regulation of these genes likely contributes to the trajectory of transcriptional events in affected tissues leading to resolution or chronicity of pain.

Duke Scholars

Author Shad Benjamin Smith Anesthesiology

Author Luda Diatchenko Anesthesiology

Published In

Pain

DOI

10.1097/j.pain.0000000000003104

EISSN

1872-6623

Publication Date

May 1, 2024

Volume

165

Issue

Start / End Page

1060 / 1073

Location

United States

Related Subject Headings

Temporomandibular Joint Disorders
Methylation
Humans
Facial Pain
Epigenesis, Genetic
Chronic Pain
Chronic Disease
Anesthesiology
52 Psychology
42 Health sciences

Citation

APA

Chicago

ICMJE

MLA

NLM

Ao, X., Parisien, M., Fillingim, R. B., Ohrbach, R., Slade, G. D., Diatchenko, L., & Smith, S. B. (2024). Whole-genome methylation profiling reveals regions associated with painful temporomandibular disorders and active recovery processes. Pain, 165(5), 1060–1073. https://doi.org/10.1097/j.pain.0000000000003104

Ao, Xiang, Marc Parisien, Roger B. Fillingim, Richard Ohrbach, Gary D. Slade, Luda Diatchenko, and Shad B. Smith. “Whole-genome methylation profiling reveals regions associated with painful temporomandibular disorders and active recovery processes.” Pain 165, no. 5 (May 1, 2024): 1060–73. https://doi.org/10.1097/j.pain.0000000000003104.

Ao X, Parisien M, Fillingim RB, Ohrbach R, Slade GD, Diatchenko L, et al. Whole-genome methylation profiling reveals regions associated with painful temporomandibular disorders and active recovery processes. Pain. 2024 May 1;165(5):1060–73.

Ao, Xiang, et al. “Whole-genome methylation profiling reveals regions associated with painful temporomandibular disorders and active recovery processes.” Pain, vol. 165, no. 5, May 2024, pp. 1060–73. Pubmed, doi:10.1097/j.pain.0000000000003104.

Ao X, Parisien M, Fillingim RB, Ohrbach R, Slade GD, Diatchenko L, Smith SB. Whole-genome methylation profiling reveals regions associated with painful temporomandibular disorders and active recovery processes. Pain. 2024 May 1;165(5):1060–1073.