Fang Fang, Pan Jian, Xu Lixiao, Li Gang, Wang Jian
Institute of Pediatric Research, Children's Hospital of Soochow University, Suzhou 215003, China.
Biomed Res Int. 2015;2015:826316. doi: 10.1155/2015/826316. Epub 2015 Jan 22.
The goal of this study was to identify potential transcriptomic markers in developing ankylosing spondylitis by a meta-analysis of multiple public microarray datasets. Using the INMEX (integrative meta-analysis of expression data) program, we performed the meta-analysis to identify consistently differentially expressed (DE) genes in ankylosing spondylitis and further performed functional interpretation (gene ontology analysis and pathway analysis) of the DE genes identified in the meta-analysis. Three microarray datasets (26 cases and 29 controls in total) were collected for meta-analysis. 905 consistently DE genes were identified in ankylosing spondylitis, among which 482 genes were upregulated and 423 genes were downregulated. The upregulated gene with the smallest combined rank product (RP) was GNG11 (combined RP=299.64). The downregulated gene with the smallest combined RP was S100P (combined RP=335.94). In the gene ontology (GO) analysis, the most significantly enriched GO term was "immune system process" (P=3.46×10(-26)). The most significant pathway identified in the pathway analysis was antigen processing and presentation (P=8.40×10(-5)). The consistently DE genes in ankylosing spondylitis and biological pathways associated with those DE genes identified provide valuable information for studying the pathophysiology of ankylosing spondylitis.
本研究的目的是通过对多个公共微阵列数据集进行荟萃分析,确定强直性脊柱炎发展过程中的潜在转录组学标志物。我们使用INMEX(表达数据综合荟萃分析)程序进行荟萃分析,以确定强直性脊柱炎中持续差异表达(DE)的基因,并对荟萃分析中鉴定出的DE基因进行功能解读(基因本体分析和通路分析)。我们收集了三个微阵列数据集(共26例病例和29例对照)进行荟萃分析。在强直性脊柱炎中鉴定出905个持续DE基因,其中482个基因上调,423个基因下调。组合秩乘积(RP)最小的上调基因是GNG11(组合RP = 299.64)。组合RP最小的下调基因是S100P(组合RP = 335.94)。在基因本体(GO)分析中,最显著富集的GO术语是“免疫系统过程”(P = 3.46×10(-26))。通路分析中鉴定出的最显著通路是抗原加工和呈递(P = 8.40×10(-5))。强直性脊柱炎中持续的DE基因以及与这些DE基因相关的生物学通路为研究强直性脊柱炎的病理生理学提供了有价值的信息。
