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Deciphering the genetic and modular connections between coronary heart disease, idiopathic pulmonary arterial hypertension and pulmonary heart disease

机译:解读冠心病,特发性肺动脉高压和肺源性心脏病之间的遗传和模块联系

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Coronary heart disease ( CHD), idiopathic pulmonary arterial hypertension ( IPAH) and pulmonary heart disease ( PHD) are circulatory system diseases that may simultaneously emerge in a patient and they are often treated together in clinical practice. However, the molecular mechanisms connecting these three diseases remain unclear. In order to determine the multidimensional characteristic correlations between these three diseases based on genomic networks to aid in medical decision-making, genes from the Online Mendelian Inheritance in Man database were obtained, and applied network construction and modularized analysis were conducted. Functional enrichment analysis was conducted to explore the associations between overlapping genes, modules and pathways. A total of 29 overlapping genes and 3 common modules were identifed for the 3 diseases. Glycosphingolipid biosynthesis and the arachidonic acid metabolism are common pathways, and the biosynthetic process is suggested to be the major function involved in the three diseases. The current study reported, to the best of our knowledge for the first time, the role of glycosphingolipid biosynthesis in IPAH and PHD. The present study provided an improved understanding of the pathological mechanisms underlying CHD, IPAH and PHD. The overlapping genes, modules and pathways suggest novel areas for further research, and drug targets. The observations of the current study additionally suggest that drug indications can be broadened because of the presence of common targets.
机译:冠心病(CHD),特发性肺动脉高压(IPAH)和肺心病(PHD)是循环系统疾病,可能同时在患者中出现,并且在临床实践中经常一起治疗。但是,连接这三种疾病的分子机制仍不清楚。为了基于基因组网络确定这三种疾病之间的多维特征相关性,以帮助进行医疗决策,从在线孟德尔遗传在线数据库中获得了基因,并进行了应用网络构建和模块化分析。进行功能富集分析以探索重叠基因,模块和途径之间的关联。对于这3种疾病,共鉴定出29个重叠基因和3个通用模块。糖鞘脂的生物合成和花生四烯酸的代谢是常见的途径,生物合成过程被认为是这三种疾病的主要功能。据我们所知,本研究首次报道了糖鞘脂生物合成在IPAH和PHD中的作用。本研究提供了对冠心病,IPAH和PHD的病理机制的更好的了解。重叠的基因,模块和途径为进一步研究和药物靶向提供了新的领域。当前研究的观察结果还表明,由于存在共同的靶点,因此可以扩大药物适应症。

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