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Identifying individual differences of fluoxetine response in juvenile rhesus monkeys by metabolite profiling

机译:通过代谢物谱分析确定幼年猕猴中氟西汀反应的个体差异

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摘要

Fluoxetine is the only psychopharmacological agent approved for depression by the US Food and Drug Administration for children and is commonly used therapeutically in a variety of neurodevelopmental disorders. Therapeutic response shows high individual variability, and severe side effects have been observed. In the current study we set out to identify biomarkers of response to fluoxetine as well as biomarkers that correlate with impulsivity, a measure of reward delay behavior and potential side effect of the drug, in juvenile male rhesus monkeys. The study group was also genotyped for polymorphisms of monoamine oxidase A (MAOA), a gene that has been associated with psychiatric disorders. We used peripheral metabolite profiling of blood and cerebrospinal fluid (CSF) from animals treated daily with fluoxetine or vehicle for one year. Fluoxetine response metabolite profiles and metabolite/reward delay behavior associations were evaluated using multivariate analysis. Our analyses identified a set of plasma and CSF metabolites that distinguish fluoxetine- from vehicle-treated animals and metabolites that correlate with impulsivity. Some metabolites displayed an interaction between fluoxetine and MAOA genotype. The identified metabolite biomarkers belong to pathways that have important functions in central nervous system physiology. Biomarkers of response to fluoxetine in the normally functioning brain of juvenile nonhuman primates may aid in finding predictors of response to treatment in young psychiatric populations and in progress toward the realization of a precision medicine approach in the area of neurodevelopmental disorders.
机译:氟西汀是经美国食品和药物管理局批准用于儿童的唯一用于抑郁症的心理药物,通常用于治疗多种神经发育障碍。治疗反应显示出高的个体变异性,并且已经观察到严重的副作用。在当前的研究中,我们着手确定对氟西汀的反应的生物标志物,以及与冲动相关的生物标志物,该标志物是雄性恒河猴的冲动延迟行为和药物潜在副作用的量度。该研究小组还对单胺氧化酶A(MAOA)的多态性进行了基因分型,该基因与精神疾病有关。我们使用每天用氟西汀或媒介治疗一年的动物的血液和脑脊液(CSF)进行外周代谢产物分析。使用多变量分析评估氟西汀反应代谢物谱和代谢物/奖励延迟行为关联。我们的分析确定了一组血浆和CSF代谢物,这些代谢物将氟西汀与车辆治疗的动物区分开来,并将代谢物与冲动相关。一些代谢物表现出氟西汀和MAOA基因型之间的相互作用。鉴定出的代谢物生物标志物属于在中枢神经系统生理学中具有重要功能的途径。在非人类灵长类动物正常运转的大脑中对氟西汀反应的生物标志物可能有助于寻找年轻精神病患者对治疗反应的预测指标,并且正在朝着神经发育障碍领域实现精确医学方法的方向发展。

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