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Metabolite profiling of antidepressant drug action reveals novel drug targets beyond monoamine elevation

机译:抗抑郁药作用的代谢产物分析揭示了超出单胺水平的新型药物靶标

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摘要

Currently used antidepressants elevate monoamine levels in the synaptic cleft. There is good reason to assume that this is not the only source for antidepressant therapeutic activities and that secondary downstream effects may be relevant for alleviating symptoms of depression. We attempted to elucidate affected biochemical pathways downstream of monoamine reuptake inhibition by interrogating metabolomic profiles in DBA/2Ola mice after chronic paroxetine treatment. Metabolomic changes were investigated using gas chromatography-mass spectrometry profiling and group differences were analyzed by univariate and multivariate statistics. Pathways affected by antidepressant treatment were related to energy metabolism, amino acid metabolism and hormone signaling. The identified pathways reveal further antidepressant therapeutic action and represent targets for drug development efforts. A comparison of the central nervous system with blood plasma metabolite alterations identified GABA, galactose-6-phosphate and leucine as biomarker candidates for assessment of antidepressant treatment effects in the periphery.
机译:当前使用的抗抑郁药会升高突触裂隙中的单胺水平。有充分的理由认为这不是抗抑郁治疗活性的唯一来源,并且其后继效应可能与缓解抑郁症状有关。我们试图通过询问慢性帕罗西汀治疗后DBA / 2Ola小鼠的代谢组学特征来阐明单胺再摄取抑制下游受影响的生化途径。使用气相色谱-质谱分析法研究代谢组学变化,并通过单变量和多变量统计分析组差异。抗抑郁药治疗的途径与能量代谢,氨基酸代谢和激素信号传导有关。所确定的途径揭示了进一步的抗抑郁治疗作用,并代表了药物开发工作的目标。将中枢神经系统与血浆代谢物改变进行比较后,发现GABA,半乳糖6-磷酸和亮氨酸是候选生物标志物,用于评估周围地区的抗抑郁药治疗效果。

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