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A new method for a quantitative assessment of P-glycoprotein-related multidrug resistance in tumour cells.

机译:一种定量评估肿瘤细胞中P-糖蛋白相关多重耐药性的新方法。

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摘要

A rapid, functional and quantitative diagnostic method for the estimation of the P-glycoprotein (P-gp)-dependent multidrug resistance is required in the clinical treatment of human tumours, as chemotherapy protocols and resistance-reversing agents could be applied accordingly. In the present work, by using a calcein accumulation method in combination with immunorecognition and drug-resistance studies, a new method is described for the quantitative estimation of the expression and function of the multidrug transporter. MDR1-transfected and drug-selected tumour cell lines with various levels of drug resistance were examined. The expression of P-gp and its cell-surface appearance were assessed by quantitative immunoblotting and by immunofluorescence cytometry. The transport function of the P-gp was assessed by measuring the extrusion of calcein acetoxymethyl ester (AM) with fluorometry and flow cytometry, while in parallel experiments drug resistance was directly examined in cell survival assays. The MDR1 activity factor (MAF), calculated from the calcein AM extrusion assay, is demonstrated to provide a reliable quantitative measure for MDR1 specific activity, reflecting cellular drug resistance. This relatively simple and rapid new functional P-gp assay surpasses the formerly used techniques in both sensitivity and reproducibility.
机译:在人类肿瘤的临床治疗中,需要一种快速,功能和定量的诊断方法来评估P-糖蛋白(P-gp)依赖性多药耐药性,因为可以相应地应用化学疗法方案和耐药逆转剂。在目前的工作中,通过结合钙黄绿素蓄积法与免疫识别和耐药性研究,描述了一种定量估计多药转运蛋白表达和功能的新方法。检查了MDR1转染和药物选择的具有不同水平耐药性的肿瘤细胞系。通过定量免疫印迹和免疫荧光细胞术评估P-gp的表达及其细胞表面外观。通过用荧光法和流式细胞术测量钙黄绿素乙酰氧基甲基酯(AM)的挤出来评估P-gp的转运功能,而在平行实验中,直接在细胞存活试验中检查了耐药性。由钙黄绿素AM挤压测定法计算得出的MDR1活性因子(MAF)被证明为MDR1比活性提供了可靠的定量指标,反映了细胞的耐药性。这种相对简单,快速的新功能性P-gp分析在灵敏度和可重复性方面都超过了以前使用的技术。

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