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Disease-Aging Network Reveals Significant Roles of Aging Genes in Connecting Genetic Diseases

机译:疾病衰老网络揭示了衰老基因在连接遗传疾病中的重要作用

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摘要

One of the challenging problems in biology and medicine is exploring the underlying mechanisms of genetic diseases. Recent studies suggest that the relationship between genetic diseases and the aging process is important in understanding the molecular mechanisms of complex diseases. Although some intricate associations have been investigated for a long time, the studies are still in their early stages. In this paper, we construct a human disease-aging network to study the relationship among aging genes and genetic disease genes. Specifically, we integrate human protein-protein interactions (PPIs), disease-gene associations, aging-gene associations, and physiological system–based genetic disease classification information in a single graph-theoretic framework and find that (1) human disease genes are much closer to aging genes than expected by chance; and (2) diseases can be categorized into two types according to their relationships with aging. Type I diseases have their genes significantly close to aging genes, while type II diseases do not. Furthermore, we examine the topological characters of the disease-aging network from a systems perspective. Theoretical results reveal that the genes of type I diseases are in a central position of a PPI network while type II are not; (3) more importantly, we define an asymmetric closeness based on the PPI network to describe relationships between diseases, and find that aging genes make a significant contribution to associations among diseases, especially among type I diseases. In conclusion, the network-based study provides not only evidence for the intricate relationship between the aging process and genetic diseases, but also biological implications for prying into the nature of human diseases.
机译:生物学和医学上具有挑战性的问题之一是探索遗传疾病的潜在机制。最近的研究表明,遗传疾病与衰老过程之间的关系对于理解复杂疾病的分子机制很重要。尽管已经研究了一些复杂的关联,但研究仍处于初期阶段。在本文中,我们构建了一个人类疾病衰老网络,以研究衰老基因与遗传疾病基因之间的关系。具体而言,我们将人类蛋白-蛋白相互作用(PPI),疾病-基因关联,衰老-基因关联以及基于生理系统的遗传疾病分类信息整合到一个单一的图论框架中,发现(1)人类疾病的基因很多比衰老的基因更接近偶然的预期; (2)根据疾病与衰老的关系,疾病可分为两类。 I型疾病的基因与衰老基因非常接近,而II型疾病的基因则与衰老基因非常接近。此外,我们从系统的角度检查了疾病老化网络的拓扑特征。理论结果表明,I型疾病的基因位于PPI网络的中心位置,而II型则不在。 (3)更重要的是,我们基于PPI网络定义了一种不对称的亲密关系来描述疾病之间的关系,并发现衰老的基因对疾病之间的关联做出了重要贡献,尤其是I型疾病之间的关联。总之,基于网络的研究不仅为衰老过程与遗传疾病之间的复杂关系提供了证据,而且还为揭示人类疾病的本质提供了生物学意义。

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