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首页> 外文期刊>Toxicology in vitro: an international journal published in association with BIBRA >Effect of chlorpyrifos on efflux transporter gene expression and function in caco-2 cells.
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Effect of chlorpyrifos on efflux transporter gene expression and function in caco-2 cells.

机译:毒死rif对caco-2细胞外排转运蛋白基因表达和功能的影响。

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摘要

The effect of chlorpyrifos (CPF) and its metabolite, chlorpyrifos-oxon (CPO), on multidrug resistance-1 (MDR1) gene expression and efflux transporter function in Caco-2 cells was determined. The effect of CPF and CPO on gene expression in Caco-2 cells was tested as a function of time using RT-PCR and competitive PCR (compPCR) techniques. The RT-PCR results depicted a maximal effect of CPF exposure on MDR1 expression at 8 h, which decreased at 24 h. Studies with CPO displayed an initial increase in expression at 4 h only. The compPCR assays were conducted with the CPF-treated group to quantify the changes in gene expression levels. The compPCR data confirmed and quantitated the results from the time-course study using semiquantitative RT-PCR. In addition to the gene expression studies, changes in efflux transporter function were investigated using Caco-2 cells grown on semipermeable membranes in Transwell trade mark plates. The permeability of verapamil was determined in cells treated for 8 h with CPF. Efflux ratios demonstrated that verapamil was effluxed at a higher rate from the CPF-treated cells as compared to the control group, confirming the inductive action of CPF on transporter function. These results suggest that CPF has the potential to modulate the bioavailability of drugs via changes in expression and function of membrane efflux transporters.
机译:确定了毒死rif(CPF)及其代谢产物毒死rif(CPO)对Caco-2细胞中多药耐药性1(MDR1)基因表达和外排转运蛋白功能的影响。使用RT-PCR和竞争性PCR(compPCR)技术,测试了CPF和CPO对Caco-2细胞基因表达的影响与时间的关系。 RT-PCR结果描述了CPF暴露在8 h对MDR1表达的最大影响,在24 h下降。使用CPO的研究显示仅在4小时时表达开始增加。用CPF处理组进行了compPCR分析,以定量基因表达水平的变化。 compPCR数据使用半定量RT-PCR确认并定量了时程研究的结果。除了基因表达研究外,还使用Transwell商标板上半透膜上生长的Caco-2细胞研究了外排转运蛋白功能的变化。维拉帕米的通透性在用CPF处理8小时的细胞中测定。外流比率表明,与对照组相比,维拉帕米从CPF处理的细胞中流出的速率更高,证实了CPF对转运蛋白功能的诱导作用。这些结果表明,CPF具有通过改变膜外向转运蛋白的表达和功能来调节药物生物利用度的潜力。

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