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Using the Oxytosis/Ferroptosis Pathway to Understand and Treat Age-Associated Neurodegenerative Diseases

机译:使用鼻涕/脱叶裂途径来理解和治疗年龄相关的神经变性疾病

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摘要

Oxytosis was first described over 30 years ago in nerve cells as a non-excitotoxic pathway for glutamate-induced cell death. The key steps of oxytosis, including glutathione depletion, lipoxygenase activation, reactive oxygen species accumulation, and calcium influx, were identified using a combination of chemical and genetic tools. A pathway with the same characteristics as oxytosis was identified in transformed fibroblasts in 2012 and named ferroptosis. Importantly, the pathophysiological changes seen in oxytosis and ferroptosis are also observed in multiple neurodegenerative diseases as well as in the aging brain. This led to the hypothesis that this pathway could be used as a screening tool to identify novel drug candidates for the treatment of multiple age-associated neurological disorders, including Alzheimer's disease (AD). Using this approach, we have identified several AD drug candidates, one of which is now in clinical trials, as well as new target pathways for AD.
机译:30多年前,在神经细胞中首次描述氧化是谷氨酸诱导细胞死亡的一种非兴奋性毒性途径。氧化作用的关键步骤,包括谷胱甘肽耗竭、脂氧合酶激活、活性氧累积和钙内流,都是通过化学和遗传学手段相结合来确定的。2012年,在转化的成纤维细胞中发现了一条与氧化作用具有相同特征的途径,并命名为铁下垂。重要的是,在多个神经退行性疾病以及衰老的大脑中,也观察到了氧化和铁下垂的病理生理变化。这导致了这样一种假设,即该途径可以用作筛选工具,以确定治疗多种年龄相关神经疾病(包括阿尔茨海默病(AD))的新候选药物。利用这种方法,我们已经确定了几种AD候选药物,其中一种正在进行临床试验,以及新的AD靶向途径。

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