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Establishment and phenotyping of disease model cells created by cell-resealing technique

机译:细胞重封技术建立的疾病模型细胞的建立和表型

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摘要

Cell-based assays are growing in importance for screening drugs and investigating their mechanisms of action. Most of the assays use so-called “normal” cell strain because it is difficult to produce cell lines in which the disease conditions are reproduced. In this study, we used a cell-resealing technique, which reversibly permeabilizes the plasma membrane, to develop diabetic (Db) model hepatocytes into which cytosol from diabetic mouse liver had been introduced. Db model hepatocytes showed several disease-specific phenotypes, namely disturbance of insulin-induced repression of gluconeogenic gene expression and glucose secretion. Quantitative image analysis and principal component analysis revealed that the ratio of phosphorylated Akt (pAkt) to Akt was the best index to describe the difference between wild-type and Db model hepatocytes. By performing image-based drug screening, we found pioglitazone, a PPARγ agonist, increased the pAkt/Akt ratio, which in turn ameliorated the insulin-induced transcriptional repression of the gluconeogenic gene phosphoenolpyruvate carboxykinase 1. The disease-specific model cells coupled with image-based quantitative analysis should be useful for drug development, enabling the reconstitution of disease conditions at the cellular level and the discovery of disease-specific markers.
机译:基于细胞的测定法对于筛选药物和研究其作用机理的重要性正日益提高。大多数测定法都使用所谓的“正常”细胞株,因为很难产生可复制疾病状况的细胞系。在这项研究中,我们使用了一种可逆性透化质膜的细胞再封闭技术,开发了已引入糖尿病小鼠肝脏细胞溶质的糖尿病(Db)模型肝细胞。 Db模型肝细胞显示出几种疾病特异性表型,即胰岛素诱导的抑制糖异生基因表达和葡萄糖分泌的紊乱。定量图像分析和主成分分析表明,磷酸化Akt(pAkt)与Akt的比率是描述野生型和Db模型肝细胞之间差异的最佳指标。通过基于图像的药物筛选,我们发现PPARγ激动剂吡格列酮增加了pAkt / Akt比率,从而改善了胰岛素诱导的糖异生基因磷酸烯醇丙酮酸羧激酶1的转录抑制。疾病特异性模型细胞与图像结合基于基因的定量分析对于药物开发,在细胞水平上重建疾病状况和发现疾病特异性标记物应该是有用的。

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