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长春新碱从多药耐药P388白血病细胞中的主动外排动力学分析。

Kinetic analysis of active efflux of vincristine from multidrug-resistant P388 leukemia cells.

作者信息

Inaba M, Watanabe T, Sugiyama Y

出版信息

Jpn J Cancer Res. 1987 Apr;78(4):397-404.

PMID:3108219
Abstract

Kinetic analysis of vincristine transport in parental and multidrug-resistant P388 leukemia cells was attempted by indirect assessment of its efflux. Practically, the initial velocity and steady-state level of vincristine uptake by ATP-depleted cells, and its steady-state level in untreated cells, were measured. As a result, a saturable process of not only influx but also efflux of vincristine was observed for the first time with both cell lines, suggesting the existence of a carrier-mediated system for influx and efflux. With increasing extracellular drug concentrations, the contribution of the mediated transport to the total flux was decreased and that of the unsaturable process, that is, simple diffusion, was increased. It should be particularly noted that the Km and Vmax values of efflux in the resistant cells were significantly less and greater, respectively, than those of the sensitive cells, providing a biochemical basis for enhanced efflux as a mechanism of multidrug-resistance. No significant difference in kinetic parameters of vincristine influx and intracellular binding contributing to resistance was found between the two cell lines.

摘要

通过间接评估长春新碱的外排,尝试对亲代和多药耐药的P388白血病细胞中长春新碱的转运进行动力学分析。实际上,测量了ATP耗竭细胞摄取长春新碱的初始速度和稳态水平,以及未处理细胞中长春新碱的稳态水平。结果,首次在两种细胞系中均观察到长春新碱的摄取和外排均为可饱和过程,这表明存在介导摄取和外排的载体系统。随着细胞外药物浓度的增加,介导转运对总通量的贡献降低,而不饱和过程(即简单扩散)的贡献增加。应特别指出的是,耐药细胞中外排的Km和Vmax值分别明显低于和高于敏感细胞,这为作为多药耐药机制的外排增强提供了生化基础。在两种细胞系之间,未发现长春新碱摄取和细胞内结合的动力学参数对耐药性有显著差异。

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