Parkinson’s disease is the second largest neurodegenerative disease worldwide and is caused by a combination of genetics and environment. It is characterized by the death of neurons in the substantia nigra of the brain but is not solely a disease of the brain, as it affects multiple tissues and organs. Studying Parkinson’s disease in accessible tissues such as skin and blood has increased our understanding of the disease’s pathogenesis. Here, we used lymphoblast cell lines generated from Parkinson’s disease patient and healthy age- and sex-matched control groups and obtained their whole-cell transcriptomes and proteomes. Our analysis revealed, in both the transcriptomes and the proteomes of PD cells, a global downregulation of genes involved in protein synthesis, as well as the upregulation of immune processes and sphingolipid metabolism. In contrast, we discovered an uncoupling of mRNA and protein expression in processes associated with mitochondrial respiration in the form of a general downregulation in associated transcripts and an upregulation in proteins. Complex V was different to the other oxidative phosphorylation complexes in that the levels of its associated transcripts were also lower, but the levels of their encoded polypeptides were not elevated. This may suggest that further layers of regulation specific to Complex V are in play.
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机译:帕金森病是全球第二大神经退行性疾病,是由遗传和环境共同引起的。它的特征是大脑黑质中的神经元死亡,但不仅仅是大脑的疾病,因为它会影响多个组织和器官。在皮肤和血液等可接近组织中研究帕金森病增加了我们对疾病发病机制的理解。在这里,我们使用了帕金森病患者和健康年龄和性别匹配的对照组产生的淋巴母细胞系,并获得了他们的全细胞转录组和蛋白质组。我们的分析显示,在 PD 细胞的转录组和蛋白质组中,参与蛋白质合成的基因整体下调,以及免疫过程和鞘脂代谢的上调。相比之下,我们发现 mRNA 和蛋白质表达在与线粒体呼吸相关的过程中以相关转录物的一般下调和蛋白质上调的形式解偶联。复合物 V 与其他氧化磷酸化复合物的不同之处在于其相关转录物的水平也较低,但其编码的多肽的水平没有升高。这可能表明特定于复合物 V 的进一步调节层正在发挥作用。
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