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成人健康与帕金森病特定过渡阶段鱼藤酮介导模型:对迟发性神经退行性疾病模型的影响。

Adult health and transition stage-specific rotenone-mediated model of Parkinson's disease: Impact on late-onset neurodegenerative disease models.

作者信息

Ayajuddin Mohamad, Phom Limamanen, Koza Zevelou, Modi Priyanka, Das Abhik, Chaurasia Rahul, Thepa Abuno, Jamir Nukshimenla, Neikha Kelevikho, Yenisetti Sarat Chandra

机构信息

Drosophila Neurobiology Laboratory, Department of Zoology, Nagaland University (Central), Lumami, India.

出版信息

Front Mol Neurosci. 2022 Aug 9;15:896183. doi: 10.3389/fnmol.2022.896183. eCollection 2022.

Abstract

Parkinson's disease (PD) affects almost 1% of the population worldwide over the age of 50 years. Exposure to environmental toxins like paraquat and rotenone is a risk factor for sporadic PD which constitutes 95% of total cases. Herbicide rotenone has been shown to cause Parkinsonian symptoms in multiple animal models. is an excellent model organism for studying neurodegenerative diseases (NDD) including PD. The aging process is characterized by differential expression of genes during different life stages. Hence it is necessary to develop life-stage-matched animal models for late-onset human disease(s) such as PD. Such animal models are critical for understanding the pathophysiology of age-related disease progression and important to understand if a genotropic drug/nutraceutical can be effective during late stages. With this idea, we developed an adult life stage-specific (health and transition phase, during which late-onset NDDs such as PD sets in) rotenone-mediated model of idiopathic PD. is susceptible to rotenone in dose-time dependent manner. Rotenone-mediated fly model of sporadic PD exhibits mobility defects (independent of mortality), inhibited mitochondrial complex I activity, dopaminergic (DAergic) neuronal dysfunction (no loss of DAergic neuronal number; however, reduction in rate-limiting enzyme tyrosine hydroxylase (TH) synthesis), and alteration in levels of dopamine (DA) and its metabolites; 3,4-Dihydroxyphenylacetic acid (DOPAC) and Homovanilic acid (HVA) in brain-specific fashion. These PD-linked behaviors and brain-specific phenotypes denote the robustness of the present fly model of PD. This novel model will be of great help to decipher life stage-specific genetic targets of small molecule mediated DAergic neuroprotection; understanding of which is critical for formulating therapeutic strategies for PD.

摘要

帕金森病(PD)影响着全球50岁以上近1%的人口。接触百草枯和鱼藤酮等环境毒素是散发性PD的一个风险因素,散发性PD占总病例的95%。除草剂鱼藤酮已被证明在多种动物模型中会引发帕金森症状。果蝇是研究包括PD在内的神经退行性疾病(NDD)的优秀模式生物。衰老过程的特征是在不同生命阶段基因的差异表达。因此,有必要为诸如PD等迟发性人类疾病建立与生命阶段相匹配的动物模型。这样的动物模型对于理解与年龄相关疾病进展的病理生理学至关重要,对于理解基因导向药物/营养保健品在疾病后期是否有效也很重要。基于这一想法,我们开发了一种成年生命阶段特异性(健康和转变阶段,在此期间诸如PD等迟发性NDD开始出现)鱼藤酮介导的特发性PD果蝇模型。果蝇对鱼藤酮的反应呈剂量-时间依赖性。鱼藤酮介导的散发性PD果蝇模型表现出运动缺陷(与死亡率无关)、线粒体复合物I活性受抑制、多巴胺能(DAergic)神经元功能障碍(DAergic神经元数量无损失;然而,限速酶酪氨酸羟化酶(TH)合成减少),以及大脑特异性方式下多巴胺(DA)及其代谢物3,4-二羟基苯乙酸(DOPAC)和高香草酸(HVA)水平的改变。这些与PD相关的行为和大脑特异性表型表明了当前PD果蝇模型的稳健性。这个新模型将极大地有助于解读小分子介导的DAergic神经保护的生命阶段特异性遗传靶点;对其的理解对于制定PD的治疗策略至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a2be/9398202/3f93d8dab896/fnmol-15-896183-g001.jpg

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