氧化应激,年龄相关性神经变性,以及神经营养治疗的潜力。

L R Williams
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引用次数: 0

摘要

肌萎缩性侧索硬化症、帕金森氏病和阿尔茨海默病是主要的人类神经退行性疾病,其病因尚不清楚。尽管在这三种疾病中都有一个独特的神经元子集受到特别的影响,但它们有几个有趣的重叠相似之处。证据支持这一假设,即这些疾病是由于氧化应激导致的自由基累积损伤无法保护造成的。如果氧化应激是这些疾病病因的基础或加剧,那么有效减弱脑组织脂质过氧化或以其他方式限制自由基损伤的药物可能为治疗这些神经退行性疾病带来希望。虽然抗氧化化学补充可能提供有效的治疗,但对神经退行性疾病最有效的治疗可能是使用特定的神经营养,促进生存的蛋白质治疗。例如,脑源性神经营养因子促进脊髓运动神经元和中脑多巴胺能神经元的存活。这些蛋白质发挥保护作用的一种机制可能是通过刺激内源性防御氧化应激和自由基损伤。这一假设正在几个实验室进行测试,并为基础神经生物学研究和治疗药物发现提供了令人兴奋的方向。
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Oxidative stress, age-related neurodegeneration, and the potential for neurotrophic treatment.

Amyotrophic lateral sclerosis, Parkinson's disease, and Alzheimer's disease are major human neurodegenerative disorders, the etiologies for which remain unknown. Although a unique subset of neurons is particularly affected in each of the three diseases, they have several intriguing overlapping similarities. Evidence is reviewed supporting the hypothesis that these diseases result from an inability to protect against accumulated damage by free radicals due to oxidative stress. If oxidative stress underlies or exacerbates the etiology of these diseases, then agents that effectively attenuate brain tissue lipid peroxidation or otherwise limit free radical damage may hold promise for the treatment of these neurodegenerative diseases. Although antioxidant chemical supplementation may provide effective therapy, the most effective therapy for neurodegenerative diseases may be treatment with specific neurotrophic, survival-promoting proteins. For example, brain-derived neurotrophic factor promotes survival of spinal motor neurons and mesencephalic dopaminergic neurons. One mechanism through which these proteins may exert their protection may be by stimulating endogenous defenses against oxidative stress and damage by free radicals. This hypothesis is being tested in several laboratories and provides exciting direction both for basic neurobiological research and therapeutic drug discovery.

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