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From the Cover: The implications of human metabolic network topology for disease comorbidity

机译:从封面开始:人类代谢网络拓扑结构对疾病合并症的影响

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摘要

Most diseases are the consequence of the breakdown of cellular processes, but the relationships among genetic/epigenetic defects, the molecular interaction networks underlying them, and the disease phenotypes remain poorly understood. To gain insights into such relationships, here we constructed a bipartite human disease association network in which nodes are diseases and two diseases are linked if mutated enzymes associated with them catalyze adjacent metabolic reactions. We find that connected disease pairs display higher correlated reaction flux rate, corresponding enzyme-encoding gene coexpression, and higher comorbidity than those that have no metabolic link between them. Furthermore, the more connected a disease is to other diseases, the higher is its prevalence and associated mortality rate. The network topology-based approach also helps to uncover potential mechanisms that contribute to their shared pathophysiology. Thus, the structure and modeled function of the human metabolic network can provide insights into disease comorbidity, with potentially important consequences for disease diagnosis and prevention.
机译:大多数疾病是细胞过程破坏的结果,但是遗传/表观遗传缺陷,它们背后的分子相互作用网络以及疾病表型之间的关系仍然知之甚少。为了深入了解这种关系,在这里我们构建了一个两方的人类疾病关联网络,其中节点是疾病,并且如果与它们相关的突变酶催化相邻的代谢反应,则将两种疾病联系在一起。我们发现,与彼此之间没有代谢联系的疾病相比,相连的疾病对显示出更高的相关反应通量率,相应的酶编码基因共表达和更高的合并症。此外,疾病与其他疾病的联系越紧密,其患病率和相关死亡率就越高。基于网络拓扑的方法还有助于发现有助于其共享病理生理的潜在机制。因此,人类代谢网络的结构和建模功能可以提供对疾病合并症的见解,对疾病的诊断和预防具有潜在的重要后果。

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