Issue title: Molecular Biology of Post Traumatic Stress
Disorder
Article type: Research Article
Authors: Uddin, Monica | Galea, Sandro | Chang, Shun-Chiao | Aiello, Allison E. | Wildman, Derek E. | de los Santos, Regina | Koenen, Karestan C.
Affiliations: Department of Epidemiology, University of Michigan
School of Public Health, Ann Arbor, MI, USA | Department of Epidemiology, Mailman School of Public
Health, Columbia University, NY, USA | Departments of Society, Human Development, and Health
and Epidemiology, Harvard School of Public Health, Boston, MA, USA and the
Center on the Developing Child, Harvard University, Cambridge, MA, USA | Center for Molecular Medicine and Genetics, Wayne
State University School of Medicine, Detroit, MI, USA
Note: [] Corresponding author: Monica Uddin, PhD, Assistant Research
Scientist, Dept. of Epidemiology, University of Michigan School of Public
Health, 1415 Washington Heights, Ann Arbor, MI, 48109, USA. Tel.: +1 734 647
9859; E-mail: [email protected]
Abstract: As potential regulators of DNA accessibility and activity,
epigenetic modifications offer a mechanism by which the environment can
moderate the effects of genes. To date, however, there have been relatively few
studies assessing epigenetic modifications associated with post-traumatic
stress disorder (PTSD). Here we investigate PTSD-associated methylation
differences in 33 genes previously shown to differ in whole blood-derived gene
expression levels between those with vs. without the disorder. Drawing on DNA
samples similarly obtained from whole blood in 100 individuals, 23 with and 77
without lifetime PTSD, we used methylation microarray data to assess whether
these 33 candidate genes showed epigenetic signatures indicative of increased
risk for, or resilience to, PTSD. Logistic regression analyses were performed
to assess the main and interacting effects of candidate genes' methylation
values and number of potentially traumatic events (PTEs), adjusting for age and
other covariates. Results revealed that only one candidate gene – MAN2C1}
– showed a significant methylation x PTE interaction, such that those
with both higher MAN2C1 methylation and greater exposure to PTEs showed a
marked increase in risk of lifetime PTSD (OR 4.35, 95% CI: 1.07, 17.77,
p=0.04). These results indicate that MAN2C1 methylation levels modify
cumulative traumatic burden on risk of PTSD, and suggest that both gene
expression and epigenetic changes at specific loci are associated with this
disorder.
Keywords: Epigenetics, psychiatric epidemiology, trauma, interaction, genomics
DOI: 10.3233/DMA-2011-0750
Journal: Disease Markers, vol. 30, no. 2-3, pp. 111-121, 2011
Received 14 April 2011
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Accepted 14 April 2011
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Published: 2011
