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首页> 外文期刊>British Journal of Pharmacology >Effects of grapefruit juice and orange juice components on P-glycoprotein- and MRP2-mediated drug efflux
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Effects of grapefruit juice and orange juice components on P-glycoprotein- and MRP2-mediated drug efflux

机译:葡萄柚汁和橙汁成分对P-糖蛋白和MRP2介导的药物外流的影响

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摘要

1. We investigated the effects of grapefruit juice (GFJ) and orange juice (OJ) on drug transport by MDR1 P-glycoprotein (P-gp) and multidrug resistance protein 2 (MRP2), which are efflux transporters expressed in human small intestine. 2. We examined the transcellular transport and uptake of [~3H]vinblastine (VBL) and [~(14)C]saquinavir in a human colon carcinoma cell line (Caco-2) and in porcine kidney epithelial cell lines transfected with human MDR1 cDNA and human MRP2 cDNA, LLC-GA5-COL150, and LLC-MRP2, respectively. 3.In Caco-2 cells, the basal-to-apical transports of [~3H]VBL and [~(14)C]saquinavir were greater than those in the opposite direction. The ratio of basal-to-apical transport to apical-to-basal transport of [~3H]VBL and [~(14)C]saquinavir by Caco-2 cells was reduced in the presence of MK571 (MRPs inhibitor), verapamil (P-gp inhibitor), cyclosporin A (inhibitor of both), 50% ethyl acetate extracts of GFJ and OJ, or their components (6′,7′-dihydroxybergamottin, bergamottin, tangeretin, hepatomethoxyfla-vone, and nobiletin). 4. Studies of transport and uptake of [~3H]VBL and [~(14)C]saquinavir with MDR1 and MRP2 transfectants showed that VBL and saquinavir are transported by both P-gp and MRP2. GFJ and OJ components inhibited the transport by MRP2 as well as P-gp. However, their inhibitory potencies for P-gp or MRP2 were substrate-dependent. 5 .The present study has revealed that GFJ and OJ interact with not only P-gp but also MRP2, both of which are expressed at apical membranes and limit the apical-to-basal transport of VBL and saquinavir in Caco-2 cells.
机译:1.我们研究了葡萄柚汁(GFJ)和橙汁(OJ)通过MDR1 P-糖蛋白(P-gp)和多药抗性蛋白2(MRP2)转运药物的作用,MDR1 P-糖蛋白和多药耐药蛋白2在人小肠中表达。 2.我们研究了人结肠癌细胞系(Caco-2)和转染人MDR1的猪肾上皮细胞系中[〜3H]长春碱(VBL)和[〜(14)C]沙奎那韦的细胞转运和摄取cDNA和人MRP2 cDNA,分别为LLC-GA5-COL150和LLC-MRP2。 3.在Caco-2细胞中,[〜3H] VBL和[〜(14)C]沙奎那韦的基底向顶部的转运大于相反方向的转运。在存在维拉帕米的MK571(MRPs抑制剂)存在下,Caco-2细胞降低了[〜3H] VBL和[〜(14)C]沙奎那韦的基础到顶部的运输与顶部到基础的运输的比率。 P-gp抑制剂),环孢菌素A(两者均是抑制剂),GFJ和OJ的50%乙酸乙酯提取物或其成分(6',7'-二羟基佛手柑,佛手柑,橘皮素,肝甲氧基黄酮和Nobiletin)。 4.对带有MDR1和MRP2转染子的[〜3H] VBL和[〜(14)C]沙奎那韦的转运和摄取的研究表明,VBL和沙奎那韦同时被P-gp和MRP2转运。 GFJ和OJ成分抑制了MRP2和P-gp的转运。但是,它们对P-gp或MRP2的抑制能力取决于底物。 5.本研究表明,GFJ和OJ不仅与P-gp相互作用,而且还与MRP2相互作用,二者均在顶膜表达,并限制了Vaco和沙奎那韦在Caco-2细胞中的顶向基底转运。

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