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首页> 外文期刊>Liver international : >Multidrug resistance associated protein 2 mediates transport of prostaglandin E.
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Multidrug resistance associated protein 2 mediates transport of prostaglandin E.

机译:多药耐药相关蛋白2介导前列腺素E的转运。

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Background/Aim: Inactivation of prostaglandin E(2) (PGE(2)) in the liver is a rapid process and occurs mainly through beta-oxidation in the peroxisome of the hepatocyte. Biliary excretion of PGE(2) is also a means of elimination from the liver. We investigated the role of multidrug resistance-associated protein 2 (MRP2) in the transport of PGE(2). Methods: Biliary PGE(2) elimination was measured in liver perfusions in Wistar and MRP2-deficient TR(-) rats. Furthermore, transport experiments were performed in membrane vesicles from human MRP2-infected Spodoptera frugiperda 21 (Sf21) insect cells. Results: The liver perfusions showed a 3.5 times higher percentage of undegraded [(3)H]PGE(2) in bile of Wistar rats in comparison with MRP2 deficient (TR(-)) rats (3.6% vs. 1.1%, respectively; P<0.05). MRP2-mediated transport of the model substrate [(3)H]DNP-SG was inhibited by PGE(2). Half maximal inhibition was achieved at a concentration of approximately 15 muM PGE(2). In addition, [(3)H]PGE(2) uptake in these vesicles was detected, and determined to be ATP dependent. Conclusion: MRP2 mediates the transport of PGE(2) and its breakdown products. The biliary excretion of PGE(2) via MRP2 may contribute to rapid elimination of the prostaglandin but might also serve to relay prostaglandin signalling to the biliary tree.
机译:背景/目的:肝脏中前列腺素E(2)(PGE(2))的失活是一个快速过程,主要通过肝细胞过氧化物酶体中的β-氧化而发生。 PGE(2)的胆汁排泄也是从肝脏清除的一种手段。我们调查了多药耐药相关蛋白2(MRP2)在PGE(2)的运输中的作用。方法:在Wistar和MRP2缺陷型TR(-)大鼠的肝脏灌注中测量胆道PGE(2)的消除。此外,运输实验是在膜囊泡中进行的,该膜囊泡感染了受人MRP2感染的草地贪夜蛾21(Sf21)昆虫细胞。结果:与MRP2缺乏(TR(-))大鼠相比,肝灌注显示Wistar大鼠胆汁中未降解[[3)H] PGE(2)的比例高3.5倍(分别为3.6%和1.1%; P <0.05)。 MRP2介导的模型底物[(3)H] DNP-SG的运输被PGE(2)抑制。在约15μMPGE(2)的浓度下达到最大抑制一半。另外,在这些囊泡中检测到[(3)H] PGE(2)摄取,并确定为依赖ATP。结论:MRP2介导PGE(2)及其分解产物的转运。 PGE(2)通过MRP2的胆汁排泄可能有助于迅速消除前列腺素,但也可能将前列腺素信号转导至胆管树。

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