首页> 外文期刊>Journal of Neural Transmission >Genomic and proteomic study to survey the mechanism of action of the anti-Parkinson’s disease drug, rasagiline compared with selegiline, in the rat midbrain
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Genomic and proteomic study to survey the mechanism of action of the anti-Parkinson’s disease drug, rasagiline compared with selegiline, in the rat midbrain

机译:基因组和蛋白质组学研究,在大鼠中脑中研究抗帕金森氏病药物雷沙吉兰和司来吉兰的作用机理

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摘要

The novel anti-Parkinson’s disease (PD) drug, rasagiline (N-propargyl-1-(R)-aminoindan), is a second generation of irreversible selective inhibitor of monoamine oxidase-B follows selegiline. In light of the recent large clinical study (phase III ADAGIO) reporting benefits in PD patients, it has been suggested that rasagiline could be the first PD treatment to receive the label neuroprotective “disease-modifying” drug. Indeed, rasagiline has been shown to have a broad neuroprotective activity against a variety of neurotoxins in preclinical models of neurodegenerative diseases and in cultured neuronal cells. In the present study, we have investigated the status of various molecular and biochemical markers in the rat midbrain following chronic treatments with rasagiline and selegiline, using proteomic and genomic analyses. Our findings demonstrated significant molecular changes induced by both drugs, at the protein and transcriptional levels, associated with neuronal differentiation, cell survival and death pathways, metabolism/oxidation stress, signaling system, and biomarkers of neurodegenerative disorders, which may be reflected in the clinical studies.
机译:新型抗帕金森氏病(PD)药物雷沙吉兰(N-propargyl-1-(R)-氨基茚满)是继司来吉兰之后的第二代不可逆选择性单胺氧化酶B抑制剂。鉴于最近的一项大型临床研究(III期ADAGIO)报道了PD患者的获益,有人提出雷沙吉兰可能是第一个接受标记神经保护性“疾病修饰”药物的PD治疗。实际上,在神经退行性疾病的临床前模型和培养的神经元细胞中,雷沙吉兰已显示出对多种神经毒素具有广泛的神经保护活性。在本研究中,我们使用蛋白质组学和基因组分析研究了雷沙吉兰和司来吉兰长期治疗后大鼠中脑各种分子和生化标志物的状况。我们的发现表明,这两种药物在蛋白质和转录水平上均引起了显着的分子变化,与神经元分化,细胞存活和死亡途径,代谢/氧化应激,信号系统和神经退行性疾病的生物标志物有关。学习。

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