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首页> 外文期刊>Free Radical Biology and Medicine: The Official Journal of the Oxygen Society >N-acetyl-L-methionyl-L-Dopa-methyl ester as a dual acting drug that relieves L-Dopa-induced oxidative toxicity.
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N-acetyl-L-methionyl-L-Dopa-methyl ester as a dual acting drug that relieves L-Dopa-induced oxidative toxicity.

机译:N-乙酰基-L-甲硫酰基-L-多巴甲基酯是一种双效药物,可减轻L-多巴引起的氧化毒性。

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摘要

Initiation and progression of Parkinson's disease seem to be linked to oxidative stress, closely related to decreased mitochondrial functions and ubiquitin proteasome system dysfunction. To date, L-Dopa is the most effective medication , although long-term treatment can enhance oxidative stress and accelerate the degenerative process of residual cells. Therefore the inhibition of oxidation of L-Dopa/dopamine and the inhibition of reactive oxygen species formation are important strategies for neuroprotective therapy. Recently, several dual acting drugs, in which L-Dopa/dopamine are covalently linked to antioxidant molecules, were shown to induce sustained delivery of both L-Dopa/dopamine in rat plasma and striatum, suggesting that these compounds might be proposed as useful agents against Parkinson's disease. Here, by analyzing GSH levels and heme oxygenase-1 expression, we investigated in primary mesencephalic neuron cultures and in newborn mice the effects of the treatment with Ac-Met-LD-OMe. Moreover, by using proteasome inhibitor-treated mice as Parkinson's disease animal model, we demonstrated the beneficial effects of the systemic administration of this novel codrug.
机译:帕金森氏病的发生和发展似乎与氧化应激有关,与线粒体功能降低和泛素蛋白酶体系统功能障碍密切相关。迄今为止,L-Dopa是最有效的药物,尽管长期治疗可以增强氧化应激并加速残留细胞的退化过程。因此,抑制L-多巴/多巴胺的氧化和抑制活性氧的形成是神经保护疗法的重要策略。最近,几种双作用药物(其中L-多巴/多巴胺与抗氧化剂分子共价连接)被证明可诱导L-多巴/多巴胺在大鼠血浆和纹状体中持续传递,这表明这些化合物可能被提议作为有用的药物对抗帕金森氏病。在这里,我们通过分析GSH水平和血红素加氧酶1的表达,研究了原发性中脑神经元培养物和新生小鼠中Ac-Met-LD-OMe的治疗效果。此外,通过使用蛋白酶体抑制剂治疗的小鼠作为帕金森氏病动物模型,我们证明了这种新型药物的全身给药的有益作用。

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