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首页> 外文期刊>European neuropsychopharmacology: the journal of the European College of Neuropsychopharmacology >Proteomic analysis of rat hippocampus and frontal cortex after chronic treatment with fluoxetine or putative novel antidepressants: CRF1 and NK1 receptor antagonists.
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Proteomic analysis of rat hippocampus and frontal cortex after chronic treatment with fluoxetine or putative novel antidepressants: CRF1 and NK1 receptor antagonists.

机译:氟西汀或推定的新型抗抑郁药:CRF1和NK1受体拮抗剂长期治疗后大鼠海马和额叶皮层的蛋白质组学分析。

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摘要

Chronic administration of antidepressants is required for their efficacy, suggesting the involvement of long-term modifications. As the impact of antidepressant treatment on the brain molecular machinery is not completely understood, we performed a proteomic analysis of rat hippocampus and frontal cortex after chronic treatment with fluoxetine, with an NK1 receptor antagonist, GR205171, and a CRF receptor 1 antagonist, DMP696. After 2D electrophoresis, protein expression levels were compared with both univariate and multivariate statistical analyses and identified by mass spectrometry. All treatments modified levels of actin isoforms, whereas both fluoxetine and GR205171 reduced synapsin II. Fluoxetine treatment increased ERK2 and NP25 and decreased vacuolar ATP synthase. After GR205171 treatment, protein disulphide isomerase A was reduced; dynamin 1 and aldose reductase increased. DMP696 modulated DRP2, pyruvate kinase, LDH and ATP synthase. Although each compound induced a specific pattern of proteinmodulation, data suggest that antidepressants share the ability of modulating neural plasticity.
机译:长期服用抗抑郁药是其疗效所必需的,这提示需要长期修饰。由于尚未完全了解抗抑郁药治疗对大脑分子机制的影响,因此我们在用氟西汀,NK1受体拮抗剂GR205171和CRF受体1拮抗剂DMP696进行慢性治疗后,对大鼠海马和额叶皮层进行了蛋白质组学分析。二维电泳后,将蛋白质表达水平与单变量和多变量统计分析进行比较,并通过质谱进行鉴定。所有治疗均改变了肌动蛋白同工型的水平,而氟西汀和GR205171均降低了突触蛋白II。氟西汀治疗增加ERK2和NP25并降低液泡ATP合酶。 GR205171处理后,蛋白质二硫键异构酶A减少;发电机1和醛糖还原酶增加。 DMP696调节DRP2,丙酮酸激酶,LDH和ATP合酶。尽管每种化合物都能诱导特定的蛋白质调节模式,但数据表明抗抑郁药具有调节神经可塑性的能力。

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