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核苷转运系统可能参与吡柔比星被HL60细胞而非单核细胞摄取的过程。

Possibility of contribution of nucleoside transport systems to pirarubicin uptake by HL60 cells but not mononuclear cells.

作者信息

Nagasawa K, Ohnishi N, Yokoyama T

机构信息

Department of Hospital Pharmacy, Faculty of Pharmaceutical Sciences, Kyoto Pharmaceutical University.

出版信息

Jpn J Cancer Res. 1998 Jun;89(6):673-80. doi: 10.1111/j.1349-7006.1998.tb03270.x.

Abstract

Previously, we reported that pirarubicin (THP), an anthracycline, was taken up, at least in part, by both human leukemic HL60 cells and mononuclear cells (MNCs) via a carrier-mediated system. In this study, the possibility of a contribution of nucleoside transport systems to the uptake of THP by HL60 cells and MNCs was investigated. The experiments were performed after both types of cells had been pretreated with a metabolic inhibitor, 2,4-dinitrophenol, to deplete cellular ATP. In HL60 cells, THP uptake was increased and decreased significantly by treatment with equilibrative nucleoside transport inhibitors, nitrobenzylthioinosine (NBMPR), nitrobenzylthioguanosine and dilazep, in the presence and absence, respectively, of an inwardly directed Na+-gradient. THP uptake by HL60 cells showed an overshoot in the presence of the gradient, and was decreased by treatment of the cells with monensin, indicating that the uptake partially depended on the Na+-gradient. In HL60 cells in which equilibrative nucleoside transport was inhibited by NBMPR, THP uptake in the presence of the gradient was inhibited by Na+-dependent concentrative nucleoside transport inhibitors, but no inhibition was observed in the absence of the gradient. In MNCs, conversely, there was no effect of any equilibrative nucleoside transport inhibitor or the Na+-gradient on THP uptake. These results suggested that THP was taken up, at least in part, via both equilibrative and concentrative nucleoside transport systems in HL60 cells, but not in MNCs.

摘要

此前,我们报道过阿霉素吡柔比星(THP)至少部分是通过载体介导系统被人白血病HL60细胞和单核细胞(MNC)摄取的。在本研究中,我们调查了核苷转运系统对HL60细胞和MNC摄取THP的贡献可能性。在用代谢抑制剂2,4-二硝基苯酚预处理两种细胞以耗尽细胞ATP后进行实验。在HL60细胞中,分别在存在和不存在内向Na+梯度的情况下,用平衡核苷转运抑制剂硝基苄基硫代肌苷(NBMPR)、硝基苄基硫代鸟苷和双嘧达莫处理,THP摄取分别显著增加和减少。HL60细胞对THP的摄取在存在梯度时出现过冲现象,并且用莫能菌素处理细胞后摄取减少,这表明摄取部分依赖于Na+梯度。在被NBMPR抑制平衡核苷转运的HL60细胞中,在存在梯度的情况下,THP摄取被Na+依赖性浓缩核苷转运抑制剂抑制,但在不存在梯度时未观察到抑制作用。相反,在MNC中,任何平衡核苷转运抑制剂或Na+梯度对THP摄取均无影响。这些结果表明,THP至少部分是通过HL60细胞中的平衡和浓缩核苷转运系统摄取的,但在MNC中并非如此。

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本文引用的文献

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