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首页> 外文期刊>Proteomics. Clinical applications >The contribution of proteomic studies in humans, animal models, and after antidepressant treatments to investigate the molecular neurobiology of major depression
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The contribution of proteomic studies in humans, animal models, and after antidepressant treatments to investigate the molecular neurobiology of major depression

机译:蛋白质组学研究在人体,动物模型和抗抑郁药物治疗中的贡献研究重大抑郁的分子神经生物学

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The neurobiological basis of major depressive disorder (MDD) is only partially understood. The proposed hypotheses postulate dysregulations of monoaminergic and other neurotransmitter pathways, impaired stress responses, insufficient neurogenetic and neurotrophic processes generating maladaptive neuroplasticity, inappropriate inflammatory and metabolic responses. Proteomic approaches can provide useful contributions to the investigation of the molecular neurobiology of MDD due to their open-ended nature. Studies performed in brain regions of MDD patients which had received antidepressant (AD) treatment showed that affected proteins mainly belonged to energy pathways, transport of molecules, signaling, and synaptic transmission. Studies performed in animal models offer the advantage of more controlled experimental conditions at the expense of potential loss in relevance. The design of proteomic investigations included experiments carried out in MDD models, in naive animals treated with ADs, and in animal models subjected to AD treatments. A comparison of results suggested an overlap of several modulated pathways between MDD patients and animal models. Examples include the regulation of energy metabolism, especially oxidative phosphorylation and glycolysis, signal transduction pathways, including calcium-calmodulin kinase II, synaptic proteins, and cytoskeletal proteins. Nevertheless, the paucity of studies performed in human brains requires additional studies to confirm the correspondence.
机译:主要抑郁症(MDD)的神经生理基础仅部分地理解。提出的假设假设单氨基能和其他神经递质途径的呼吸困难,压力响应受损,神经发生和神经营养过程不足,产生不良神经塑性,不适当的炎症和代谢反应。蛋白质组学方法可以为其开放性质的开放性质的分子神经生物学提供有用的贡献。在接受抗抑郁药(AD)治疗的MDD患者的脑区域中进行的研究表明,受影响的蛋白质主要属于能量途径,分子运输,信号传播和突触传递。在动物模型中进行的研究以潜在的相关性损失为代价提供了更受控实验条件的优势。蛋白质组学研究的设计包括在用广告治疗的幼稚动物中进行MDD模型中进行的实验,并在进行AD治疗的动物模型中。结果的比较表明MDD患者和动物模型之间的几种调制途径的重叠。实例包括能量代谢的调节,尤其是氧化磷酸化和糖酵解,信号转导途径,包括钙 - 钙调霉素激酶II,突触蛋白和细胞骨架蛋白。然而,人类大脑中进行的研究缺乏需要额外的研究以确认对应关系。

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