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一种膜活性剂对源自“原发性”和“转移性”生长的Lewis肺癌细胞摄取阿霉素的影响。

Effect of a membrane-active agent on uptake of adriamycin in Lewis lung carcinoma cells derived from 'primary' and 'metastatic' growths.

作者信息

Bar-Shira-Maymon B, Michowitz M, Gibli O, Klein O, Pinchasov A, Leibovici J

机构信息

Department of Pathology, Sackler Faculty of Medicine, Tel-Aviv University, Israel.

出版信息

Chemotherapy. 1992;38(1):66-73. doi: 10.1159/000238943.

DOI:10.1159/000238943
PMID:1618005
Abstract

The treatment of metastatic growth still constitutes a challenge for cancer research. Tumor progression is often accompanied by a loss in sensitivity to previously efficient drugs. Decreased intracellular accumulation of cytotoxic agents is probably the major reason for drug resistance, although other mechanisms have also been described. Properties of the cell membrane have been shown to determine the metastatic phenotype. This cellular organelle is also responsible for the multiple drug resistance phenomenon. Membrane-active agents may increase cell permeability to drugs, counteracting thereby drug resistance. In the present study the effect of the nonionic detergent Tween 80 on sensitivity to adriamycin (ADR) of cells derived from Lewis lung carcinoma 'primary tumors' (PT)-the local growth following subcutaneous inoculation - and 'metastatic tumors' (MT) - lung tumors which develop following intravenous injection - was compared. Flow cytometry analysis demonstrated several differences between cells derived from the PT and the MT: (1) single ADR treatment showed that MT cells possessed a lower percentage of a high ADR permeability subpopulation than PT cells; (2) a dose-dependent shift to a higher ADR accumulating population was seen in the presence of Tween 80 for both cell types. However, the increase in percentage of high ADR permeability cells was more pronounced in MT (up to x4.7) than in PT (up to x1.3) cells. This differential effect of the membrane-acting agent was evident at various ADR (10-50 micrograms) and Tween 80 (0.1-0.4%) concentrations. The present results corroborate previous data obtained in our group in another tumor progression model, AKR lymphoma.

摘要

转移性肿瘤生长的治疗仍是癌症研究面临的一项挑战。肿瘤进展常常伴随着对先前有效药物敏感性的丧失。细胞毒性药物细胞内蓄积减少可能是耐药的主要原因,不过也有其他机制的报道。细胞膜特性已被证明可决定转移表型。这种细胞器也与多药耐药现象有关。膜活性剂可增加细胞对药物的通透性,从而对抗耐药性。在本研究中,比较了非离子去污剂吐温80对源自Lewis肺癌“原发性肿瘤”(PT,皮下接种后的局部生长)和“转移性肿瘤”(MT,静脉注射后形成的肺部肿瘤)细胞阿霉素(ADR)敏感性的影响。流式细胞术分析显示源自PT和MT的细胞存在若干差异:(1)单次ADR处理表明,MT细胞中高ADR通透性亚群的百分比低于PT细胞;(2)对于两种细胞类型,在吐温80存在的情况下均可见剂量依赖性地向更高ADR蓄积群体转变。然而,MT细胞(高达4.7倍)中高ADR通透性细胞百分比的增加比PT细胞(高达1.3倍)更明显。在各种ADR(10 - 50微克)和吐温80(0.1 - 0.4%)浓度下,这种膜活性剂的差异效应均很明显。本研究结果证实了我们小组在另一种肿瘤进展模型AKR淋巴瘤中获得的先前数据。

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