Major depressive disorder (MDD) in children and adolescents is a recurrent and disabling condition globally but its pathophysiology remains poorly elucidated and there are limited effective treatments available. We performed metabolic profiling of plasma samples based on ultra-high-performance liquid chromatography equipped with quadrupole time-offlight mass spectrometry to explore the potential biomarkers of depression in children and adolescents with MDD. We identified several perturbed pathways, including fatty acid metabolism-particularly the polyunsaturated fatty acids metabolism, and purine metabolism-that were associated with MDD in these young patients. In addition, inosine was shown as a potential independent diagnostic biomarker for MDD, achieving an area under the ROC curve of 0.999 in discriminating drug-naive MDD patients and 0.866 in discriminating drug-treated MDD from healthy controls. Moreover, we found evidence for differences in the pathophysiology of MDD in children and adolescents to that of adult MDD, specifically with tryptophan metabolism. Through metabolomic analysis, we have identified links between a framework of metabolic perturbations and the pathophysiology and diagnostic biomarker of child and adolescent MDD.
Antidepressant medication has a small overall effect in reducing depression in young patients with combined depressive and substance-use disorders, but does not appear to improve substance use outcomes.
New generation antidepressant therapies, including serotonin-norepinephrine reuptake
inhibitor (SNRIs), were introduced in the late 1980s; however, few comprehensive
studies have compared the benefits and risks of various contemporary treatments for
major depressive disorder (MDD) in young patients. A comprehensive literature search
of PubMed, Cochrane, Embase, Web of Science, and PsycINFO databases was conducted
from 1970 to January 2015. Only clinical trials that randomly assigned one SNRI or
placebo to patients aged 7 to 18 years who met the diagnostic criteria for major
depressive disorder were included. Treatment success, dropout rate, and suicidal
ideation/attempt outcomes were measured. Primary efficacy was determined by pooling
the risk ratios (RRs) of treatment response and remission. Acceptability was
determined by pooling the RRs of dropouts for all reasons and for adverse effects as
well as suicide-risk outcomes. Five trials with a total of 973 patients were
included. SNRIs were not significantly more effective than placebo for treatment
response but were for remission. The comparison of patients taking SNRIs that dropped
out for all reasons and those taking placebo did not reach statistical significance.
Significantly more patients taking SNRIs dropped out for adverse effects than those
taking placebo. No significant difference was found in suicide-related risk outcomes.
SNRI therapy does not display a superior efficacy and is not better tolerated
compared to placebo in these young patients. However, duloxetine has a potential
beneficial effect for depression in young populations, showing a need for further
research.
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