| Literature DB >> 28103696 |
Bendik S Winsvold1,2, Priit Palta3,4, Else Eising5, Christian M Page2,6, Arn Mjm van den Maagdenberg5,7, Aarno Palotie3,8,9,10,11,12, John-Anker Zwart1,2.
Abstract
Background The biological mechanisms of headache chronification are poorly understood. We aimed to identify changes in DNA methylation associated with the transformation from episodic to chronic headache. Methods Participants were recruited from the population-based Norwegian HUNT Study. Thirty-six female headache patients who transformed from episodic to chronic headache between baseline and follow-up 11 years later were matched against 35 controls with episodic headache. DNA methylation was quantified at 485,000 CpG sites, and changes in methylation level at these sites were compared between cases and controls by linear regression analysis. Data were analyzed in two stages (Stages 1 and 2) and in a combined meta-analysis. Results None of the top 20 CpG sites identified in Stage 1 replicated in Stage 2 after multiple testing correction. In the combined meta-analysis the strongest associated CpG sites were related to SH2D5 and NPTX2, two brain-expressed genes involved in the regulation of synaptic plasticity. Functional enrichment analysis pointed to processes including calcium ion binding and estrogen receptor pathways. Conclusion In this first genome-wide study of DNA methylation in headache chronification several potentially implicated loci and processes were identified. The study exemplifies the use of prospectively collected population cohorts to search for epigenetic mechanisms of disease.Entities:
Keywords: Chronic headache; cohort studies; epigenetics
Mesh:
Year: 2017 PMID: 28103696 DOI: 10.1177/0333102417690111
Source DB: PubMed Journal: Cephalalgia ISSN: 0333-1024 Impact factor: 6.292