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首页> 外文期刊>Life sciences >Effects of grapefruit juice on the multidrug transporter P-glycoprotein in the human proximal tubular cell line HK-2.
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Effects of grapefruit juice on the multidrug transporter P-glycoprotein in the human proximal tubular cell line HK-2.

机译:葡萄柚汁对人近端肾小管细胞株HK-2中多药转运蛋白P-糖蛋白的影响。

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摘要

The multidrug transporter MDR-1 P-glycoprotein (Pgp) has been recently pointed out as an important mechanism underlying chemical interaction between drugs and many commonly ingested substances, including grapefruit juice (GFJ). Modulation of intestinal Pgp dependent transport by GFJ may lead to changes in bioavailability of drugs that are substrates of Pgp itself, by affecting their presystemic clearance. Since other cellular sites expressing Pgp and devoted to drug disposition, like kidney proximal tubules, could be involved in these pharmacokinetic interactions, we investigated the effect of GFJ on the expression and activity of Pgp in the human immortalized tubular cell line HK-2. Two flavonoid compounds related to GFJ, kaempferol and naringenin, were also tested for their effects on HK-2 Pgp. HK-2 cells cultured for 4 days in the presence of GFJ, showed a dose-dependent decrease in Pgp immunoblottable amount as well as a decrease in MDR-1 mRNA level, as shown by western blot analysis and RT-PCR, respectively. Both kaempferol and naringenin were also able to significantly decrease Pgp immunoblottable amount. To test whether the downregulation of HK-2 Pgp due to GFJ exposition could influence the cell sensitivity to drugs that are transported by Pgp itself, HK-2 cells precultured with GFJ were exposed to scalar concentrations of Cyclosporin A or Vinblastine and cell viability examined 36 hours later. The cytotoxicity of both drugs was increased. The calcein-AM test in untreated cells showed that GFJ, kaempferol or naringenin inhibited Pgp activity. Downregulation of Pgp as well inhibition of its function by GFJ or its related components in tubular cells could have a role in changing disposition kinetics of some important therapeutic agents.
机译:最近已经指出,多药转运蛋白MDR-1 P-糖蛋白(Pgp)是药物与许多常用摄入物质(包括葡萄柚汁(GFJ))之间化学相互作用的重要机制。 GFJ对肠道Pgp依赖性转运的调节可能会通过影响药物的系统前清除率而导致药物本身的生物利用度发生变化。由于其他表达Pgp并致力于药物处置的细胞位点(如肾近端小管)可能参与这些药代动力学相互作用,因此我们研究了GFJ对人永生化肾小管细胞株HK-2中Pgp表达和活性的影响。还测试了两种与GFJ有关的类黄酮化合物,kaempferol和naringenin对HK-2 Pgp的作用。在GFJ存在下培养4天的HK-2细胞分别表现出剂量依赖性的Pgp免疫印迹量降低和MDR-1 mRNA水平降低,如分别通过蛋白质印迹分析和RT-PCR所示。山emp酚和柚皮素都能够显着降低Pgp免疫印迹量。为了测试GFJ暴露导致HK-2 Pgp的下调是否会影响细胞对Pgp自身转运的药物的敏感性,将预先接种GFJ的HK-2细胞暴露于标量浓度的环孢菌素A或长春花碱,并检测了细胞活力几个小时以后。两种药物的细胞毒性均增加。未处理细胞中的钙黄绿素-AM测试表明,GFJ,山奈酚或柚皮素抑制Pgp活性。 Pgp的下调以及GFJ或其在肾小管细胞中的相关成分对其功能的抑制可能在改变某些重要治疗剂的处置动力学中起作用。

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