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首页> 外文期刊>British Journal of Cancer >Regulation of initial vinblastine influx by P-glycoprotein
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Regulation of initial vinblastine influx by P-glycoprotein

机译:P-糖蛋白对长春花碱初始流入的调节

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P-glycoprotein (PGP) is an energy-dependent efflux pump that serves to protect cells against the cytotoxicity of many natural product drugs including vinblastine (VBL). In this study we investigated the role of PGP in regulating initial VBL influx. The apparent influx of VBL, measured over the first 20 s, was 2-fold lower in KB-GRC1 cells expressing a transfected mdr1 gene at high level than in non-expressing parental KB-3-1 cells. Inhibition of PGP efflux function with dipyridamole increased the influx rate constant by 4.0-fold in the KB-GRC1 cells but only 2.1-fold in the KB-3-1 cells. Verapamil, another inhibitor of PGP-mediated efflux, increased the initial influx rate constant by 2.7-fold in the KB-GRC1 cells but only 1.4-fold in the KB-3-1 cells. Inhibition of PGP function by depletion of ATP increased influx by 6.8-fold and 2.2-fold in the two cell types, respectively. Mutation of PGP at both ATP binding sites abolished its ability to limit initial influx. Thus, VBL is serving as an efficient substrate for the efflux pump even within the first few seconds of drug exposure, consistent with the hypothesis that PGP may directly efflux drug from the cell membrane.
机译:P-糖蛋白(PGP)是一种能量依赖型外排泵,用于保护细胞免受包括长春碱(VBL)在内的许多天然产物药物的细胞毒性。在这项研究中,我们调查了PGP在调节初始VBL流入中的作用。在前20 s内测得的VBL的表观流入量在高水平表达转染mdr1基因的KB-GRC1细胞中比不表达的亲本KB-3-1细胞低2倍。用潘生丁抑制PGP外排功能使KB-GRC1细胞的流入速率常数增加了4.0倍,而KB-3-1细胞仅使流入速率常数增加了2.1倍。维拉帕米,另一种PGP介导的外流抑制剂,在KB-GRC1细胞中使初始流入速率常数增加了2.7倍,而在KB-3-1细胞中仅增加了1.4倍。在两种细胞类型中,通过消耗ATP抑制PGP功能的流入分别增加了6.8倍和2.2倍。在两个ATP结合位点的PGP突变取消了其限制初始流入的能力。因此,即使在药物暴露的最初几秒钟内,VBL仍可作为外排泵的有效底物,这与PGP可能直接从细胞膜外排药物的假设相一致。

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