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Protein localization as a principal feature of the etiology and comorbidity of genetic diseases

机译:蛋白质定位是遗传疾病的病因和合并症的主要特征

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摘要

Proteins targeting the same subcellular localization tend to participate in mutual protein–protein interactions (PPIs) and are often functionally associated. Here, we investigated the relationship between disease-associated proteins and their subcellular localizations, based on the assumption that protein pairs associated with phenotypically similar diseases are more likely to be connected via subcellular localization. The spatial constraints from subcellular localization significantly strengthened the disease associations of the proteins connected by subcellular localizations. In particular, certain disease types were more prevalent in specific subcellular localizations. We analyzed the enrichment of disease phenotypes within subcellular localizations, and found that there exists a significant correlation between disease classes and subcellular localizations. Furthermore, we found that two diseases displayed high comorbidity when disease-associated proteins were connected via subcellular localization. We newly explained 7584 disease pairs by using the context of protein subcellular localization, which had not been identified using shared genes or PPIs only. Our result establishes a direct correlation between protein subcellular localization and disease association, and helps to understand the mechanism of human disease progression.
机译:靶向相同亚细胞定位的蛋白质倾向于参与蛋白质间相互作用(PPI),并且通常在功能上相关。在这里,我们基于与表型相似疾病相关的蛋白质对更可能通过亚细胞定位连接的假设,研究了疾病相关蛋白与其亚细胞定位之间的关系。来自亚细胞定位的空间限制显着增强了通过亚细胞定位连接的蛋白质的疾病关联。特别地,某些疾病类型在特定的亚细胞定位中更为普遍。我们分析了亚细胞定位内疾病表型的富集,发现疾病类别与亚细胞定位之间存在显着相关性。此外,我们发现当疾病相关蛋白通过亚细胞定位连接时,两种疾病显示出较高的合并症。我们通过使用蛋白质亚细胞定位的背景新解释了7584种疾病对,而仅使用共享基因或PPI尚未发现。我们的结果建立了蛋白质亚细胞定位与疾病关联之间的直接关联,并有助于了解人类疾病进展的机制。

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