OXTR-Related Markers in Clinical Depression: a Longitudinal Case–Control Psychotherapy Study

We investigated stability and change of plasma and urinary oxytocin as well as OXTR DNA methylation patterns through psychotherapy. Furthermore, we explored the potential impact of inpatient psychotherapy on oxytocin-related biomarkers and vice versa by differentiating patients who remitted from dep...

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Bibliographic Details
Published in:Journal of molecular neuroscience 2022-04, Vol.72 (4), p.695-707
Main Authors: Reiner, Iris C., Gimpl, Gerald, Beutel, Manfred E., Bakermans-Kranenburg, Marian J., Frieling, Helge
Format: Article
Language:English
Subjects:
Adult
Antidepressants
Biomarkers
Biomedical and Life Sciences
Biomedicine
Bisulfite
Case-Control Studies
Cell Biology
Deoxyribonucleic acid
Depression - genetics
Depression - therapy
DNA
DNA Methylation
Female
Humans
Mental depression
Middle Aged
Neurochemistry
Neurology
Neurosciences
Oxytocin
Oxytocin - genetics
Oxytocin - metabolism
Patients
Plasma levels
Proteomics
Psychotherapy
Receptors, Oxytocin - genetics
Receptors, Oxytocin - metabolism
Urine
Young Adult
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Summary:We investigated stability and change of plasma and urinary oxytocin as well as OXTR DNA methylation patterns through psychotherapy. Furthermore, we explored the potential impact of inpatient psychotherapy on oxytocin-related biomarkers and vice versa by differentiating patients who remitted from depression versus non-remitters. Blood and urine samples were taken from 85 premenopausal women (aged 19–52), 43 clinically depressed patients from a psychosomatic inpatient unit, and 42 healthy control subjects matched for age and education at two points of time. Serum and urine oxytocin were measured using standard ELISA, and DNA methylation of the OXTR gene was assessed using bisulfite sequencing at the time of admission (baseline) and at discharge and from controls at matched time points. Oxytocin plasma levels were not associated with depression and were influenced by neither time in healthy controls nor psychotherapy in patients. Non-remitting depressed patients had significantly lower oxytocin urine levels before and after psychotherapy treatment. We found significantly lower exon 1 OTXR methylation in depressed patients over time and these differences were driven by patients remitting due to psychotherapy. A reverse pattern — higher levels of methylation in remitters — was found for exon 2 OXTR DNA methylation. Plasma oxytocin, urinary oxytocin, and OXTR DNA methylation patterns were intrapersonally relatively stable. OXTR -related factors were seemingly unaffected by inpatient psychotherapeutic treatment, but we found significant differences between remitting and non-remitting patients in urinary oxytocin and OXTR DNA methylation. If replicated, this suggests that OXTR -related markers may predict inpatient treatment outcomes of clinically depressed patients.
ISSN:0895-8696
1559-1166
DOI:10.1007/s12031-021-01930-7