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首页> 外文期刊>BioMed research international >Rapid Identification of Potential Drugs for Diabetic Nephropathy Using Whole-Genome Expression Profiles of Glomeruli
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Rapid Identification of Potential Drugs for Diabetic Nephropathy Using Whole-Genome Expression Profiles of Glomeruli

机译:使用全基因组表达型肾小球糖尿病肾病潜在药物的快速鉴定

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Objective. To investigate potential drugs for diabetic nephropathy (DN) using whole-genome expression profiles and the Connectivity Map (CMAP). Methodology. Eighteen Chinese Han DN patients and six normal controls were included in this study. Whole-genome expression profiles of microdissected glomeruli were measured using the Affymetrix human U133 plus 2.0 chip. Differentially expressed genes (DEGs) between late stage and early stage DN samples and the CMAP database were used to identify potential drugs for DN using bioinformatics methods. Results. (1) A total of 1065 DEGs (FDR < 0.05 and fold change > 1.5) were found in late stage DN patients compared with early stage DN patients. (2) Piperlongumine, 15d-PGJ2 (15-delta prostaglandin J2), vorinostat, and trichostatin A were predicted to be the most promising potential drugs for DN, acting as NF-κB inhibitors, histone deacetylase inhibitors (HDACIs), PI3K pathway inhibitors, or PPARy agonists, respectively. Conclusion. Using whole-genome expression profiles and the CMAP database, we rapidly predicted potential DN drugs', and therapeutic potential was confirmed by previously published studies. Animal experiments and clinical trials are needed to confirm both the safety and efficacy of these drugs in the treatment of DN.
机译:客观的。使用全基因组表达谱和连接图(CMAP)来研究糖尿病肾病(DN)的潜在药物。方法。本研究纳入了十八中的中国汉族人和六种正常对照。使用Affymetrix人U133加2.0芯片测量微放射肾小球的全基因组表达谱。晚期和早期DN样品之间的差异表达基因(DEGS)和CMAP数据库用于使用生物信息化方法识别DN的潜在药物。结果。 (1)与早期DN患者相比,在晚期DN患者中,共有1065次(FDR <0.05和折叠变化> 1.5)。 (2)Piperlongumine,15d-PGJ2(15Δ前列腺素J2),vorinostat和richostatina预计是DN最有希望的潜在药物,作为NF-κB抑制剂,组蛋白脱乙酰酶抑制剂(HDACIS),PI3K途径抑制剂或分别的ppary激动剂。结论。使用全基因组表达谱和CMAP数据库,我们迅速预测潜在的DN药物,并通过先前公布的研究证实了治疗潜力。需要动物实验和临床试验来证实这些药物在DN治疗中的安全性和功效。

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