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Cited 8 time in webofscience Cited 10 time in scopus
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Circulating Serum MicroRNAs as Potential Diagnostic Biomarkers of Posttraumatic Stress Disorder: A Pilot Studyopen access

Authors
Snijders, ClaraKrauskopf, JulianPishva, EhsanEijssen, LarsMachiels, BarbieKleinjans, JosKenis, Guntervan den Hove, DanielKim, Myeong OkBoks, Marco P. M.Vinkers, Christiaan H.Vermetten, EricGeuze, ElbertRutten, Bart P. F.de Nijs, Laurence
Issue Date
22-Nov-2019
Publisher
FRONTIERS MEDIA SA
Keywords
posttraumatic stress disorder; circulating miRNAs; diagnostic biomarker; trauma; susceptibility
Citation
FRONTIERS IN GENETICS, v.10
Indexed
SCIE
SCOPUS
Journal Title
FRONTIERS IN GENETICS
Volume
10
URI
https://scholarworks.bwise.kr/gnu/handle/sw.gnu/8502
DOI
10.3389/fgene.2019.01042
ISSN
1664-8021
Abstract
Posttraumatic stress disorder (PTSD) is a psychiatric disorder that can develop upon exposure to a traumatic event. While most people are able to recover promptly, others are at increased risk of developing PTSD. However, the exact underlying biological mechanisms of differential susceptibility are unknown. Identifying biomarkers of PTSD could assist in its diagnosis and facilitate treatment planning. Here, we identified serum microRNAs (miRNAs) of subjects that underwent a traumatic event and aimed to assess their potential to serve as diagnostic biomarkers of PTSD. Next-generation sequencing was performed to examine circulating miRNA profiles of 24 members belonging to the Dutch military cohort Prospective Research in Stress-Related Military Operations (PRISMO). Three groups were selected: "susceptible" subjects who developed PTSD after combat exposure, "resilient" subjects without PTSD, and nonexposed control subjects (N = 8 per group). Differential expression analysis revealed 22 differentially expressed miRNAs in PTSD subjects compared to controls and 1 in PTSD subjects compared to resilient individuals (after multiple testing correction and a log2 fold-change cutoff of >=|1|). Weighted Gene Coexpression Network Analysis (WGCNA) identified a module of coexpressed miRNAs which could distinguish between the three groups. In addition, receiver operating characteristic curve analyses suggest that the miRNAs with the highest module memberships could have a strong diagnostic accuracy as reflected by high areas under the curves. Overall, the results of our pilot study suggest that serum miRNAs could potentially serve as diagnostic biomarkers of PTSD, both individually or grouped within a cluster of coexpressed miRNAs. Larger studies are now needed to validate and build upon these preliminary findings.
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