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Microarray and Bioinformatics Analysis of Gene Expression in Experimental Membranous Nephropathy

机译:实验性膜性肾病基因表达的微阵列和生物信息学分析

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摘要

Background: Passive Heymann nephritis (PHN), the best characterized animal model of experimental membranous nephropathy, is characterized by subepithelial immune deposits, podocyte foot processes effacement and massive proteinuria beginning 4 days following disease induction. Although single genes involved in PHN have been studied, no whole genome-wide expression analysis of kidney tissue has been performed. Methods: Microarray analysis was performed to identify gene expression changes in PHN rat kidneys during the onset of proteinuria. Results: Our results showed that 234 transcripts were differentially expressed in diseased animals compared to controls. Genes exclusively upregulated in diseased animals were mainly required for cell structure and motility, immunity and defense, cell cycle, and developmental processes. The single most increased gene was transgelin (Tagln) showing a 70-fold upregulation in animals with PHN. Protein-protein interaction analysis revealed the following four processes of major relevance in disease manifestation: (i) DNA damage and repair; (ii) changes in the extracellular matrix; (iii) deregulation of cytokines and growth factors, as well as (iv) rearrangements of the cy-toskeleton. Conclusion: We show for the first time the complex interplay between multiple different genes in experimental membranous nephropathy, supporting a role for genomic approaches to better understanding and definingSpecific disease processes.
机译:背景:被动性Heymann肾炎(PHN)是实验性膜性肾病的最典型动物模型,其特征在于上皮下免疫沉积,足细胞足突脱落和疾病诱导后4天开始大量蛋白尿。尽管已经研究了参与PHN的单个基因,但尚未对肾脏组织进行全基因组范围的表达分析。方法:进行微阵列分析以鉴定蛋白尿发作期间PHN大鼠肾脏中的基因表达变化。结果:我们的结果表明,与对照组相比,患病动物中234个转录物差异表达。在患病动物中专门上调的基因主要是细胞结构和运动,免疫与防御,细胞周期和发育过程所需的。增幅最大的单一基因是转胶蛋白(Tagln),在患有PHN的动物中表现出70倍的上调。蛋白质-蛋白质相互作用分析揭示了与疾病表现主要相关的以下四个过程:(i)DNA损伤和修复; (ii)细胞外基质的变化; (iii)细胞因子和生长因子的失控,以及(iv)细胞骨架的重排。结论:我们首次展示了实验性膜性肾病中多个不同基因之间的复杂相互作用,支持了基因组学方法对更好地理解和定义特定疾病过程的作用。

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