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Microtubule-targeting anticancer drug eribulin induces drug efflux transporter P-glycoprotein

机译:靶向微管的抗癌药物eribulin诱导药物外流转运蛋白P-糖蛋白

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摘要

This study examined the effects of microtubule-targeting anticancer drugs (paclitaxel, cabazitaxel, and eribulin) on the expression of drug efflux transporter P-glycoprotein, which is encoded by . Paclitaxel and eribulin induced promoter activity in a concentration-dependent manner, while cabazitaxel had little effect in human intestinal epithelial LS174T cells. Overexpression of the nuclear receptor pregnane X receptor (PXR) gene ( ) enhanced paclitaxel- and eribulin-induced activation, but expression of the nuclear receptor co-repressor silencing mediator for retinoid and thyroid receptors (SMRT) gene ( ) repressed activation. Eribulin increased the mRNA and protein expression of P-glycoprotein in LS174T cells. Cellular uptake of rhodamine 123 and calcein-acetoxymethyl ester (calcein-AM), P-glycoprotein substrates, decreased in paclitaxel- or eribulin-treated LS174T cells. Eribulin also increased promoter activity in human breast cancer MCF7 cells. The results suggest that the microtubule-targeting anticancer drug eribulin can induce the drug efflux transporter P-glycoprotein via PXR in human intestinal and breast cancer cells and thus influence the efficacy of anticancer drugs.
机译:这项研究检查了靶向微管的抗癌药物(紫杉醇,卡巴他赛和埃布林)对药物外排转运蛋白P糖蛋白表达的影响,该蛋白由编码。紫杉醇和eribulin以浓度依赖的方式诱导启动子活性,而卡巴他赛对人肠上皮LS174T细胞影响很小。核受体孕烷X受体(PXR)基因()的过表达增强了紫杉醇和eribulin诱导的激活,但类视色素和甲状腺受体(SMRT)基因()的核受体共阻抑沉默介体的表达抑制了激活。 Eribulin增加LS174T细胞中P-糖蛋白的mRNA和蛋白表达。罗丹明123和钙黄绿素-乙酰氧基甲酯(钙黄绿素-AM),P-糖蛋白底物的细胞摄取在紫杉醇或eribulin处理的LS174T细胞中降低。依立布林还增加了人乳腺癌MCF7细胞中的启动子活性。结果表明,靶向微管的抗癌药物eribulin可通过PXR诱导人肠癌细胞和乳腺癌细胞中的药物外流转运蛋白P-糖蛋白,从而影响抗癌药物的功效。

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