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利用cDNA微阵列技术发现类风湿性滑膜炎中独特的基因表达谱:存在多种组织破坏和修复途径的证据

Discovery of distinctive gene expression profiles in rheumatoid synovium using cDNA microarray technology: evidence for the existence of multiple pathways of tissue destruction and repair.

作者信息

van der Pouw Kraan T C T M, van Gaalen F A, Huizinga T W J, Pieterman E, Breedveld F C, Verweij C L

机构信息

Department of Molecular Cell Biology, VU University Medical Center, Amsterdam, The Netherlands.

出版信息

Genes Immun. 2003 Apr;4(3):187-96. doi: 10.1038/sj.gene.6363975.

Abstract

Rheumatoid arthritis (RA) is a heterogeneous disease. We used cDNA microarray technology to subclassify RA patients and disclose disease pathways in rheumatoid synovium. Hierarchical clustering of gene expression data identified two main groups of tissues (RA-I and RA-II). A total of 121 genes were significantly higher expressed in the RA-I tissues, whereas 39 genes were overexpressed in the RA-II tissues. Among the 121 genes overexpressed in RA-I tissues, a relative majority of nine genes are located on chromosome 6p21.3. An interpretation of biological processes that take place revealed that the gene expression profile in RA-I tissues is indicative for an adaptive immune response. The RA-II group showed expression of genes suggestive for fibroblast dedifferentiation. Within the RA-I group, two subgroups could be distinguished; the RA-Ia group showed predominantly immune-related gene activity, while the RA-Ib group showed an additional higher activity of genes indicative for the classical pathway of complement activation. All tissues except the RA-Ia subgroup showed elevated expression of genes involved in tissue remodeling. These results confirm the heterogeneous nature of RA and suggest the existence of distinct pathogenic mechanisms that contribute to RA. The differences in expression profiles provide opportunities to stratify patients based on molecular criteria.

摘要

类风湿性关节炎(RA)是一种异质性疾病。我们使用cDNA微阵列技术对RA患者进行亚分类,并揭示类风湿滑膜中的疾病途径。基因表达数据的层次聚类确定了两组主要组织(RA-I和RA-II)。共有121个基因在RA-I组织中显著高表达,而39个基因在RA-II组织中过表达。在RA-I组织中过表达的121个基因中,相对多数的9个基因位于6号染色体的6p21.3区域。对所发生的生物学过程的解释表明,RA-I组织中的基因表达谱表明存在适应性免疫反应。RA-II组显示出提示成纤维细胞去分化的基因表达。在RA-I组中,可以区分出两个亚组;RA-Ia组主要表现出免疫相关基因活性,而RA-Ib组显示出另外更高的与补体激活经典途径相关基因的活性。除RA-Ia亚组外,所有组织中参与组织重塑的基因表达均升高。这些结果证实了RA的异质性,并提示存在导致RA的不同致病机制。表达谱的差异为基于分子标准对患者进行分层提供了机会。

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