摘要
本综述检查microRNA 7(miR-7)是否具有减缓帕金森病(PD)进展的潜力。 首先,miR-7的准确表达允许中枢神经系统中的正常发育,生理学和神经发生,同时将α-突触核蛋白(α-Syn)保持在生理水平。 其次,患有PD和帕金森病MPTP诱导的动物的患者在与多巴胺能神经变性相关的脑区域中显示出miR-7的显着降低。 临床样品的黑质中miR-7的消耗与α-Syn积聚,多巴胺能细胞的丧失和纹状体中多巴胺的减少有关。 因此,miR-7替代疗法的目标是下调α-Syn和其他PD相关基因,实现关于氧化应激的多目标益处线粒体健康,细胞糖酵解,细胞凋亡和炎症小体激活的抑制。 虽然疾病调节药物是PD临床管理的主要未满足需求,但miR-7替代疗法对神经病理学的关键机制具有显着的潜力。 这种创新性治疗将减少路易体中的α-Syn积累并保留在诊断时仍然存活的剩余神经元,从而减缓从PD的早期阶段的疾病进展,其特征在于相对轻微的运动损伤至晚期和更致残的阶段。
关键词: miR-7,帕金森病,神经变性,RNAi,MicroRNA,Synuclein,Lewy体,Synucleinopathy。
Current Gene Therapy
Title:miR-7 Replacement Therapy in Parkinson’s Disease
Volume: 18 Issue: 3
关键词: miR-7,帕金森病,神经变性,RNAi,MicroRNA,Synuclein,Lewy体,Synucleinopathy。
摘要: The present review examines whether the microRNA 7 (miR-7) holds potential for slowing Parkinson's disease (PD) progression. First, the accurate expression of miR-7 allows for normal development, physiology, and neurogenesis in the central nervous system, also keeping alpha-synuclein (α-Syn) at the physiological level. Second, patients with PD and parkinsonian MPTP-induced animals exhibit a significant decrease of miR-7 in brain areas associated with dopaminergic neurodegeneration. Depletion of miR-7 in the substantia nigra of clinical samples is related to α-Syn accumulation, loss of dopaminergic cells, and reduction of dopamine in the striatum. Therefore, the goal of a miR-7- replacement therapy is to downregulate α-Syn and other PD-related genes, achieving multi-target benefits regarding oxidative stress, mitochondrial health, cell glycolysis, apoptosis, and inhibition of inflammasome activation. While a disease-modifying drug is a major unmet need for the clinical management of PD, an miR-7-replacement therapy presents a striking potential against critical mechanisms of neuropathology. Such innovative treatment would reduce α-Syn accumulation in the Lewy bodies and preserve remaining neurons yet viable at the time of diagnosis, thus slowing disease progression from the early phase of PD characterized by a relatively mild motor impairment to an advanced and more disabling stage.
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Cite this article as:
miR-7 Replacement Therapy in Parkinson’s Disease, Current Gene Therapy 2018; 18 (3) . https://dx.doi.org/10.2174/1566523218666180430121323
DOI https://dx.doi.org/10.2174/1566523218666180430121323 |
Print ISSN 1566-5232 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-5631 |
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