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普朗尼克L61对多药耐药细胞中阿霉素的细胞毒性活性、转运及亚细胞分布的致敏作用

Hypersensitizing effect of pluronic L61 on cytotoxic activity, transport, and subcellular distribution of doxorubicin in multiple drug-resistant cells.

作者信息

Venne A, Li S, Mandeville R, Kabanov A, Alakhov V

机构信息

Immunology Research Center, Institute Armand-Frappier, University of Quebec, Laval, Canada.

出版信息

Cancer Res. 1996 Aug 15;56(16):3626-9.

PMID:8705995
Abstract

The present study demonstrated that poly(oxypropylene) and poly(oxyethylene) block copolymer pluronic L61 (L61)-hypersensitized multidrug-resistant CHRC5 Chinese hamster ovary cells and MCF-7/ADR human breast carcinoma cells to the cytotoxic action of doxorubicin (Dox). CHRC5 and MCF-7/ADR cells manifested 290- and 700-fold increases, respectively, in their sensitivity to Dox/L61 formulation compared with free Dox. Their sensitive counterparts Aux-B1 and MCF-7 displayed only marginal or no increase at all in their response to Dox/L61. The study of the drug transport performed by flow cytometry showed that L61 enhanced the drug uptake and reduced the P-glycoprotein-mediated drug efflux. Visualization of Dox subcellular distribution in CHRC5 cells by fluorescent microscopy revealed that Dox was sequestered in cytoplasmic vesicles, whereas incubation of the cells with Dox/L61 altered the drug compartmentalization by releasing the drug from these vesicles and shifting it to the nucleus. These findings suggested that the hypersensitive response of multidrug-resistant cells to the action of Dox/L61 was caused by an increase in the drug accumulation and changes in its subcellular distribution.

摘要

本研究表明,聚(氧化丙烯)和聚(氧化乙烯)嵌段共聚物普朗尼克L61(L61)使多药耐药的中国仓鼠卵巢细胞CHRC5和MCF-7/ADR人乳腺癌细胞对阿霉素(Dox)的细胞毒性作用超敏化。与游离Dox相比,CHRC5和MCF-7/ADR细胞对Dox/L61制剂的敏感性分别提高了290倍和700倍。它们的敏感对应物Aux-B1和MCF-7对Dox/L61的反应仅略有增加或根本没有增加。通过流式细胞术进行的药物转运研究表明,L61增强了药物摄取并减少了P-糖蛋白介导的药物外排。通过荧光显微镜观察CHRC5细胞中Dox的亚细胞分布,发现Dox被隔离在细胞质小泡中,而用Dox/L61孵育细胞则通过将药物从这些小泡中释放出来并将其转移到细胞核中改变了药物的区室化。这些发现表明,多药耐药细胞对Dox/L61作用的超敏反应是由药物积累的增加及其亚细胞分布的变化引起的。

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