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首页> 外文期刊>International journal of dermatology >Comparisons of gene expression in normal, lesional, and non-lesional psoriatic skin using DNA microarray techniques
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Comparisons of gene expression in normal, lesional, and non-lesional psoriatic skin using DNA microarray techniques

机译:使用DNA芯片技术比较正常,病变和非病变牛皮癣皮肤中的基因表达

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Objectives: This study was designed to explore the pathogenesis of psoriasis and to identify potential bio-targets. Genome array technology was used to analyze the gene expression profiles of lesional and non-lesional psoriatic skin samples and normal skin samples. Methods: Gene expression profile GSE14905 was downloaded from the Gene Expression Omnibus (GEO) database. This included skin biopsy samples from normal healthy donors (n = 21), lesional skin biopsy samples from psoriasis patients (n = 33), and non-lesional skin biopsy samples from psoriasis patients (n = 28). Differentially expressed genes (DEGs) were identified using the Limma package in R language. Functions of specific DEGs were predicted by Gene Ontology (GO) enrichment analysis. A protein-protein interaction network was constructed to display the interactions among common DEGs. Finally, DAVID and WebGestalt were used to achieve a functional analysis of common DEGs. Results: Totals of 1020, 562, and 643 genes, respectively, were identified as being differentially expressed in normal versus lesional, normal versus non-lesional, and lesional versus non-lesional samples. The specific DEGs in the three groups were enriched for several GO terms, including mitotic cell cycle, immune response, and response to organic matter. The 40 common DEGs in the three groups may be involved in the defense response pathway in the development of psoriasis. Furthermore, three genes (RGS1, SOCS3, and NAMPT) may play key roles in distinguishing lesional and non-lesional tissues from normal tissues, and 10 genes (PTRRC, ALDH1A3, SAMSA1, C15orf48, ZC3H12A, SOD2, IL8, LTF, RHCG, and IL7R) may play key roles in distinguishing non-lesional from normal and lesional samples. Conclusions: These genes may be considered as potential diagnostic markers and targets of therapeutics in psoriasis.
机译:目的:本研究旨在探讨牛皮癣的发病机理并确定潜在的生物靶标。基因组阵列技术用于分析皮损和非皮损牛皮癣皮肤样品和正常皮肤样品的基因表达谱。方法:基因表达谱GSE14905从Gene Expression Omnibus(GEO)数据库下载。这包括来自正常健康捐献者的皮肤活检样本(n = 21),来自牛皮癣患者的病变皮肤活检样本(n = 33)以及来自牛皮癣患者的非病变皮肤活检样本(n = 28)。使用Limma软件包以R语言识别了差异表达的基因(DEG)。通过基因本体论(GO)富集分析预测了特定DEG的功能。构建了蛋白质-蛋白质相互作用网络以显示常见DEG之间的相互作用。最后,使用DAVID和WebGestalt对常见的DEG进行功能分析。结果:在正常与病变,正常与非病变,以及病变与非病变样品中,分别鉴定出总共1020、562和643个基因差异表达。三组中的特定DEG富含多个GO术语,包括有丝分裂细胞周期,免疫应答和对有机物的应答。三组中的40种常见DEG可能参与了牛皮癣发展过程中的防御反应途径。此外,三个基因(RGS1,SOCS3和NAMPT)可能在区分病变组织和非病变组织与正常组织中起关键作用,还有10个基因(PTRRC,ALDH1A3,SAMSA1,C15orf48,ZC3H12A,SOD2,IL8,LTF,RHCG,和IL7R)可能在区分非病变样本与正常样本和病变样本中起关键作用。结论:这些基因可能被认为是牛皮癣潜在的诊断标记和治疗靶点。

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