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Hypermethylation in the ZBTB20 gene is associated with major depressive disorder

Authors :
Enda M. Byrne
Jonathan Mill
Therese M. Murphy
Xiaowei Zhu
Sara Mostafavi
Kirsten J. Ward
Jordana T. Bell
Nicholas G. Martin
Lutz Krause
Matthew N. Davies
Tim D. Spector
Honglong Wu
Jun Wang
Hanlin Lu
Pei-Chein Tsai
David A. Collier
Yuan Liu
Fei Gao
Naomi R. Wray
Emma Dempster
Anjali K. Henders
Alexis Battle
Source :
Genome Biology, Genome Biology; Vol 15
Publication Year :
2014

Abstract

Background: Although genetic variation is believed to contribute to an individual’s susceptibility to major depressive disorder, genome-wide association studies have not yet identified associations that could explain the full etiology of the disease. Epigenetics is increasingly believed to play a major role in the development of common clinical phenotypes, including major depressive disorder. Results: Genome-wide MeDIP-Sequencing was carried out on a total of 50 monozygotic twin pairs from the UK and Australia that are discordant for depression. We show that major depressive disorder is associated with significant hypermethylation within the coding region of ZBTB20, and is replicated in an independent cohort of 356 unrelated case-control individuals. The twins with major depressive disorder also show increased global variation in methylation in comparison with their unaffected co-twins. ZBTB20 plays an essential role in the specification of the Cornu Ammonis-1 field identity in the developing hippocampus, a region previously implicated in the development of major depressive disorder. Conclusions: Our results suggest that aberrant methylation profiles affecting the hippocampus are associated with major depressive disorder and show the potential of the epigenetic twin model in neuro-psychiatric disease.

Details

Language :
English
ISSN :
14656906
Database :
OpenAIRE
Journal :
Genome Biology
Accession number :
edsair.doi.dedup.....8661164195f7101f63744bdca601f902
Full Text :
https://doi.org/10.1186/gb-2014-15-4-r56