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Integrated Analyses of Gene Expression Profiles Digs out Common Markers for Rheumatic Diseases

机译:基因表达谱的综合分析找出风湿性疾病的常见标志

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Objective Rheumatic diseases have some common symptoms. Extensive gene expression studies, accumulated thus far, have successfully identified signature molecules for each rheumatic disease, individually. However, whether there exist shared factors across rheumatic diseases has yet to be tested. Methods We collected and utilized 6 public microarray datasets covering 4 types of representative rheumatic diseases including rheumatoid arthritis, systemic lupus erythematosus, ankylosing spondylitis, and osteoarthritis. Then we detected overlaps of differentially expressed genes across datasets and performed a meta-analysis aiming at identifying common differentially expressed genes that discriminate between pathological cases and normal controls. To further gain insights into the functions of the identified common differentially expressed genes, we conducted gene ontology enrichment analysis and protein-protein interaction analysis. Results We identified a total of eight differentially expressed genes (TNFSF10, CX3CR1, LY96, TLR5, TXN, TIA1, PRKCH, PRF1), each associated with at least 3 of the 4 studied rheumatic diseases. Meta-analysis warranted the significance of the eight genes and highlighted the general significance of four genes (CX3CR1, LY96, TLR5, and PRF1). Protein-protein interaction and gene ontology enrichment analyses indicated that the eight genes interact with each other to exert functions related to immune response and immune regulation. Conclusion The findings support that there exist common factors underlying rheumatic diseases. For rheumatoid arthritis, systemic lupus erythematosus, ankylosing spondylitis and osteoarthritis diseases, those common factors include TNFSF10, CX3CR1, LY96, TLR5, TXN, TIA1, PRKCH, and PRF1. In-depth studies on these common factors may provide keys to understanding the pathogenesis and developing intervention strategies for rheumatic diseases.
机译:目的风湿性疾病有一些常见症状。迄今为止积累的广泛的基因表达研究已成功地分别鉴定了每种风湿病的特征分子。但是,风湿性疾病之间是否存在共享因素尚待检验。方法我们收集并利用了6个公共微阵列数据集,涵盖了4种代表性风湿病,包括类风湿性关节炎,系统性红斑狼疮,强直性脊柱炎和骨关节炎。然后,我们在整个数据集中检测了差异表达基因的重叠,并进行了荟萃分析,旨在鉴定可区分病理病例和正常对照的常见差异表达基因。为了进一步了解已鉴定的常见差异表达基因的功能,我们进行了基因本体富集分析和蛋白质-蛋白质相互作用分析。结果我们确定了总共八个差异表达基因(TNFSF10,CX3CR1,LY96,TLR5,TXN,TIA1,PRKCH,PRF1),每个与至少4种研究的风湿病疾病中的3种相关。荟萃分析保证了这八个基因的重要性,并突出了四个基因(CX3CR1,LY96,TLR5和PRF1)的一般意义。蛋白质-蛋白质相互作用和基因本体论富集分析表明,八个基因彼此相互作用以发挥与免疫应答和免疫调节有关的功能。结论研究结果支持存在风湿性疾病的共同因素。对于类风湿关节炎,系统性红斑狼疮,强直性脊柱炎和骨关节炎疾病,这些常见因素包括TNFSF10,CX3CR1,LY96,TLR5,TXN,TIA1,PRKCH和PRF1。对这些共同因素的深入研究可能为了解风湿性疾病的发病机理和制定干预策略提供关键。

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