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对阿霉素从敏感和耐药癌细胞中的流出进行连续原位电化学监测。

Continuous in situ electrochemical monitoring of doxorubicin efflux from sensitive and drug-resistant cancer cells.

作者信息

Yi C, Gratzl M

机构信息

Department of Biomedical Engineering, Case Western Reserve University, Cleveland, Ohio 44106, USA.

出版信息

Biophys J. 1998 Nov;75(5):2255-61. doi: 10.1016/S0006-3495(98)77670-2.

Abstract

One of the least well understood problems in cancer chemotherapy is the cross-resistance of certain tumor cells to a series of chemically unrelated drugs. Multidrug resistance (MDR) can be attributed to several different biophysical processes, among them increased drug efflux. This has been found to correlate with overexpression of the cell surface 170-kDa P-glycoprotein that actively excludes cytotoxic drugs against their concentration gradient. To better understand MDR, experimental methods are needed to study drug efflux from cancer cells. Continuous measurement of efflux of nonfluorescent drugs on the same cell culture in situ, or assessing efflux from a few cells or even a single cell, is beyond the capabilities of existing technologies. In this work, a carbon fiber (CF) microelectrode is used to monitor efflux of doxorubicin from a monolayer of two cell lines: an auxotrophic mutant of Chinese hamster ovary cells, AUXB1, and its MDR subline, CHRC5. Because doxorubicin is both fluorescent and electroactive, the results could be validated against existing data obtained optically and with other techniques on the same cell lines, with good agreement found. The electrochemical detection, however, is capable of in situ monitoring with high temporal resolution and is suitable for single-cell studies.

摘要

癌症化疗中最难以理解的问题之一是某些肿瘤细胞对一系列化学结构不相关药物的交叉耐药性。多药耐药性(MDR)可归因于几种不同的生物物理过程,其中包括药物外排增加。已发现这与细胞表面170 kDa P-糖蛋白的过度表达相关,该蛋白可主动逆浓度梯度排出细胞毒性药物。为了更好地理解MDR,需要实验方法来研究癌细胞的药物外排。在原位对同一细胞培养物中的非荧光药物外排进行连续测量,或者评估少数细胞甚至单个细胞的外排,超出了现有技术的能力范围。在这项工作中,使用碳纤维(CF)微电极监测两种细胞系单层中阿霉素的外排:中国仓鼠卵巢细胞的营养缺陷型突变体AUXB1及其MDR亚系CHRC5。由于阿霉素具有荧光性和电活性,因此可以将结果与通过光学方法和其他技术在同一细胞系上获得的现有数据进行验证,结果吻合良好。然而,电化学检测能够以高时间分辨率进行原位监测,适用于单细胞研究。

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本文引用的文献

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Genetic analysis of the multidrug transporter.多药转运蛋白的遗传分析
Annu Rev Genet. 1995;29:607-49. doi: 10.1146/annurev.ge.29.120195.003135.
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Mechanism of multidrug resistance.多药耐药机制。
Biochim Biophys Acta. 1988 Aug 3;948(1):87-128. doi: 10.1016/0304-419x(88)90006-6.

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