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固相代表性差异分析中减法过程的监测:一种候选药物的表征

Monitoring of the subtraction process in solid-phase representational difference analysis: characterization of a candidate drug.

作者信息

Boräng S, Andersson T, Thelin A, Larsson M, Odeberg J, Lundeberg J

机构信息

Department of Biotechnology, KTH Royal Institute of Technology, Teknikringen 34, S-100 44 Stockholm, Sweden.

出版信息

Gene. 2001 Jun 27;271(2):183-92. doi: 10.1016/s0378-1119(01)00486-3.

Abstract

In this study, we have applied and evaluated a modified cDNA representational difference analysis (RDA) protocol based on magnetic bead technology to study the molecular effects of a candidate drug (N,N'-diacetyl-L-cystine, DiNAC) in a model for atherosclerosis. Alterations in a gene expression profile induced by DiNAC were investigated in a human monocytic cell line (THP-1) differentiated into macrophage-like cells by lipopolysaccharide and further exposed to DiNAC. Three rounds of subtraction have been performed and the difference products from the second and third rounds have been characterized in detail by analysis of over 1000 gene sequences. Two protocols for analysis of the subtraction products have been evaluated, a shotgun approach and size selection of both distinct fragments and band-patterned smear. We demonstrate that in order to obtain a representative view of the most abundant gene fragments, the shotgun procedure is preferred. The obtained sequences were analyzed against the UniGene and Expressed Gene Anatomy Database (EGAD) databases and the results were visualized and analyzed with the ExProView software enabling rapid pair-wise comparison and identification of individual genes or functional groups of genes with altered expression levels. The identified differentially expressed gene sequences were comprised of both genes with known involvement in atherosclerosis or cholesterol biosynthesis and genes previously not implicated in these processes. The applicability of a solid-phase shotgun RDA protocol, combined with virtual chip monitoring, results in new starting points for characterization of novel candidate drugs.

摘要

在本研究中,我们应用并评估了一种基于磁珠技术的改良型cDNA代表性差异分析(RDA)方案,以研究一种候选药物(N,N'-二乙酰基-L-胱氨酸,DiNAC)在动脉粥样硬化模型中的分子效应。在通过脂多糖分化为巨噬细胞样细胞并进一步暴露于DiNAC的人单核细胞系(THP-1)中,研究了DiNAC诱导的基因表达谱变化。进行了三轮消减,并通过对1000多个基因序列的分析详细表征了第二轮和第三轮的差异产物。评估了两种分析消减产物的方案,一种是鸟枪法,另一种是对不同片段和带状涂片进行大小选择。我们证明,为了获得最丰富基因片段的代表性视图,鸟枪法更为可取。将获得的序列与UniGene和表达基因解剖数据库(EGAD)进行比对分析,并使用ExProView软件对结果进行可视化和分析,该软件能够快速进行成对比较并识别表达水平发生变化的单个基因或基因功能组。鉴定出的差异表达基因序列既包括已知参与动脉粥样硬化或胆固醇生物合成的基因,也包括以前未涉及这些过程的基因。固相鸟枪法RDA方案与虚拟芯片监测相结合的适用性,为新型候选药物的表征提供了新的起点。

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