AI Article Synopsis

  • The study explores how different types of trauma affect the risk of developing PTSD through changes in DNA methylation, particularly in the NFATC1 gene.
  • Researchers found that five trauma types were linked to reduced methylation at one specific site (cg17057218) and increased methylation at another site (cg22324981).
  • The findings suggest that changes in methylation could mediate a significant portion of the relationship between some trauma types and the risk for PTSD, indicating a biological mechanism involved in this connection.

Article Abstract

The mechanisms through which exposure to differing trauma types become biologically embedded to shape the risk for post-traumatic stress disorder (PTSD) is unclear. DNA methylation (5-mC), particularly in stress-relevant genes, may play a role in this relationship. Here, we conducted path analysis using generalized structural equation modeling to investigate whether blood-derived 5-mC in Nuclear Factor of Activated T Cells 1 (NFATC1) mediates the prospective association between each of five different trauma types ("assaultive violence", "other injury or shocking experience", "learning of trauma to loved one", "sudden, unexpected death of a close friend or relative", and "other") and lifetime PTSD. All five trauma types were significantly associated with reduced methylation at NFATC1 CpG site, cg17057218. Two of the five trauma types were significantly associated with increased methylation at NFATC1 CpG site, cg22324981. Moreover, methylation at cg17057218 significantly mediated 21-32% of the total effect for four of the five trauma types, while methylation at cg22324981 mediated 27-40% of the total effect for two of the five trauma types. These CpG sites were differentially associated with transcription factor binding sites and chromatin state signatures. NFATC1 5-mC may be a potential mechanism in the relationship between some trauma types and prospective risk for PTSD.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9018623PMC
http://dx.doi.org/10.1016/j.psychres.2022.114510DOI Listing

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