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Comprehensive Gene expression meta-analysis and integrated bioinformatic approaches reveal shared signatures between thrombosis and myeloproliferative disorders

机译:综合基因表达Meta分析和集成的生物信息方法揭示血栓形成和髓鳞病症之间的共同签名

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Thrombosis is a leading cause of morbidity and mortality in patients with myeloproliferative disorders (MPDs), particularly polycythemia vera (PV) and essential thrombocythemia (ET). Despite the attempts to establish a link between them, the shared biological mechanisms are yet to be characterized. An integrated gene expression meta-analysis of five independent publicly available microarray data of the three diseases was conducted to identify shared gene expression signatures and overlapping biological processes. Using INMEX bioinformatic tool, based on combined Effect Size (ES) approaches, we identified a total of 1,157 differentially expressed genes (DEGs) (697 overexpressed and 460 underexpressed genes) shared between the three diseases. EnrichR tool's rich library was used for comprehensive functional enrichment and pathway analysis which revealed "mRNA Splicing" and "SUMO E3 ligases SUMOylate target proteins" among the most enriched terms. Network based meta-analysis identified MYC and FN1 to be the most highly ranked hub genes. Our results reveal that the alterations in biomarkers of the coagulation cascade like F2R, PROS1, SELPLG and ITGB2 were common between the three diseases. Interestingly, the study has generated a novel database of candidate genetic markers, pathways and transcription factors shared between thrombosis and MPDs, which might aid in the development of prognostic therapeutic biomarkers.
机译:血栓形成是肌酚患者(MPDS),特别是多胆症Vera(PV)和基本血小板(ET)患者发病率和死亡率的主要原因。尽管试图建立它们之间的联系,但共同的生物机制尚未表现。进行了三种疾病的五种独立公知微阵列数据的综合基因表达Meta分析,以鉴定共享基因表达签名和重叠的生物过程。使用Inmex生物信息工具,基于组合效果大小的方法,我们鉴定了三种疾病之间共有的1,157个差异表达的基因(DEGS)(697个过表达和460个缺陷的基因)。 Enrichr工具的富含库用于综合功能性富集和途径分析,揭示了最丰富的术语中的“SUMO E3拼接”和“SUMO E3 LIG酶”中的“SUMO E3 LIG酶”。基于网络的META分析确定了MYC和FN1是最高度排名的集线基因。我们的研究结果表明,在三种疾病之间,凝血级联的凝血级联的生物标志物的变化是常见的。有趣的是,该研究已经产生了血栓形成和MPDS之间共用的候选遗传标记,途径和转录因子的新型数据库,这可能有助于开发预后治疗生物标志物。

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