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维拉帕米可降低多药耐药人白血病细胞系中P-糖蛋白的表达。

Verapamil decreases P-glycoprotein expression in multidrug-resistant human leukemic cell lines.

作者信息

Muller C, Bailly J D, Goubin F, Laredo J, Jaffrézou J P, Bordier C, Laurent G

机构信息

Laboratoire de Pharmacologie et de Toxicologie Fondamentales, Toulouse, France.

出版信息

Int J Cancer. 1994 Mar 1;56(5):749-54. doi: 10.1002/ijc.2910560523.

Abstract

We studied the effect of verapamil on Pgp expression (Pgp) in MDR human leukemia cell lines, K562/ADR and CEM VLB100. In the K562/ADR cell line, addition of verapamil to the culture medium (15 microM concentration) resulted in a 3-fold decrease in Pgp expression after 72 hr exposure. The effect of verapamil was reversible, and Pgp expression reached the level of untreated controls 24 hr after discontinuation of verapamil. Similar results were obtained with the human vinblastine-resistant cell line, CEM VLB100. On the contrary, no effect on Pgp expression was observed when the cells were treated with nifedipine or diltiazem (2 other calcium-channel blockers), even at doses that inhibited cell proliferation. The level of Pgp mRNA in the presence of verapamil was measured by Northern blot and was also decreased 2-fold (with the maximum reached within 24 hr), suggesting a transcriptional or post-transcriptional mechanism for verapamil. We further established that the effect of verapamil on Pgp expression led to an increase in DNR and VLB accumulation and cytotoxicity. These results suggest that verapamil acts specifically on Pgp expression in these drug-selected leukemic cells. The identification of a potentially novel mechanism of action may provide new insights as to how chemosensitization may be more effectively applied in vivo.

摘要

我们研究了维拉帕米对多药耐药人白血病细胞系K562/ADR和CEM VLB100中P-糖蛋白(Pgp)表达的影响。在K562/ADR细胞系中,向培养基中添加维拉帕米(浓度为15微摩尔),暴露72小时后Pgp表达下降了3倍。维拉帕米的作用是可逆的,停用维拉帕米24小时后,Pgp表达恢复到未处理对照的水平。在人长春碱耐药细胞系CEM VLB100中也得到了类似结果。相反,当用硝苯地平或地尔硫䓬(另外两种钙通道阻滞剂)处理细胞时,即使在抑制细胞增殖的剂量下,也未观察到对Pgp表达有影响。用Northern印迹法检测了维拉帕米存在时Pgp mRNA的水平,其也下降了2倍(在24小时内达到最大值),提示维拉帕米作用于转录或转录后机制。我们进一步证实,维拉帕米对Pgp表达的影响导致柔红霉素(DNR)和长春碱(VLB)蓄积增加及细胞毒性增强。这些结果表明,维拉帕米在这些经药物筛选的白血病细胞中特异性作用于Pgp表达。对一种潜在新作用机制的鉴定可能为体内更有效地应用化学增敏作用提供新的见解。

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