To date, it remains impossible to guarantee that short-term treatment given to a patient
suffering from a major depressive episode (MDE) will improve long-term efficacy. Objective
biological measurements and biomarkers that could help in predicting the clinical
evolution of MDE are still warranted. To better understand the reason nearly half of MDE
patients respond poorly to current antidepressive treatments, we examined the gene
expression profile of peripheral blood samples collected from 16 severe MDE patients and
13 matched controls. Using a naturalistic and longitudinal design, we ascertained mRNA and
microRNA (miRNA) expression at baseline, 2 and 8 weeks later. On a genome-wide scale, we
detected transcripts with roles in various biological processes as significantly
dysregulated between MDE patients and controls, notably those involved in nucleotide
binding and chromatin assembly. We also established putative interactions between
dysregulated mRNAs and miRNAs that may contribute to MDE physiopathology. We selected a
set of mRNA candidates for quantitative reverse transcriptase PCR (RT-qPCR) to validate
that the transcriptional signatures observed in responders is different from
nonresponders. Furthermore, we identified a combination of four mRNAs (PPT1,
TNF, IL1B and HIST1H1E) that could be predictive of treatment
response. Altogether, these results highlight the importance of studies investigating the
tight relationship between peripheral transcriptional changes and the dynamic clinical
progression of MDE patients to provide biomarkers of MDE evolution and prognosis.
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