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首页> 外文期刊>Nature reviews. Neurology >Pathophysiological and diagnostic implications of cortical dysfunction in ALS
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Pathophysiological and diagnostic implications of cortical dysfunction in ALS

机译:ALS皮质功能障碍的病理生理学和诊断意义

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Cortical dysfunction-specifically, the development of hyperexcitability-seems to be an early and intrinsic feature of sporadic and familial amyotrophic lateral sclerosis (ALS) phenotypes, preceding the onset of lower motor neuron dysfunction and correlating with ensuing lower motor neuron dysfunction and degeneration. In fact, cortical dysfunction could provide a pathogenic basis for ALS, with corticomotor neuronal hyperexcitability mediating motor neuron degeneration via a trans-synaptic, glutamate-mediated, excitotoxic mechanism. The recent identification of C9orf72 repeat expansion as an important genetic risk factor for both ALS and frontotemporal dementia has underscored the importance of cortical function in ALS pathogenesis, and has helped to confirm that the disease forms part of a spectrum of central neurodegenerative processes. Changes in cortical function that develop in ALS could prove useful as diagnostic biomarkers, potentially enhancing the diagnosis of ALS at an early stage of the disease process. Pathophysiological and diagnostic biomarkers of cortical function might also provide insights to guide the development of future therapeutic approaches, including stem cell and genetic interventions, thereby providing potential for more-effective management of patients with ALS.
机译:特别是皮质功能障碍,过度兴奋的发展似乎是散发性和家族性肌萎缩性侧索硬化症(ALS)表型的早期和固有特征,先于下运动神经元功能障碍发作,并与随之而来的下运动神经元功能障碍和变性相关。实际上,皮质功能障碍可为ALS提供病因基础,皮质运动神经元过度兴奋性通过反突触,谷氨酸介导的兴奋性毒性机制介导运动神经元变性。 C9orf72重复扩增最近被鉴定为ALS和额颞痴呆的重要遗传危险因素,这突显了皮质功能在ALS发病机理中的重要性,并有助于证实该疾病构成了中枢神经退行性过程的一部分。在ALS中发展的皮质功能变化可能被证明可作为诊断性生物标志物,可能在疾病过程的早期增强ALS的诊断。皮质功能的病理生理学和诊断生物标志物也可能为指导未来治疗方法的发展提供见解,包括干细胞和基因干预,从而为更有效地治疗ALS患者提供了潜力。

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