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药物外排泵MRP2:在生理病理情况下以及受内源性和外源性化合物影响时的表达调控

The drug efflux pump MRP2: regulation of expression in physiopathological situations and by endogenous and exogenous compounds.

作者信息

Payen L, Sparfel L, Courtois A, Vernhet L, Guillouzo A, Fardel O

机构信息

INSERM U456, Faculté de Pharmacie, Rennes, France.

出版信息

Cell Biol Toxicol. 2002;18(4):221-33. doi: 10.1023/a:1016020626941.

Abstract

The multidrug resistance-associated protein 2 (MRP2) is an ATP-binding cassette transporter involved in biliary, renal, and intestinal secretion of numerous organic anions, including endogenous compounds such as bilirubin and exogenous compounds such as drugs and toxic chemicals. Its expression can be modulated in various physiopathological situations, notably being markedly decreased during liver cholestasis and upregulated in some cancerous tissues. In addition, MRP2 levels are altered in hepatocytes in response to hormones such as glucocorticoids and to structurally unrelated drugs such as rifampicin, phenobarbital, ritonavir, and cisplatin. The chemical carcinogen 2-acetylaminofluorene and chemopreventive agents such as oltipraz and sulforaphane also markedly increased MRP2 expression in liver parenchymal cells. Interestingly, most of the chemical inducers of MRP2 act on drug-metabolizing enzymes, indicating a coordinated regulation of these detoxifying proteins; cellular mechanisms involved are, at least partly, common and may be related to nuclear hormone receptors such as the pregnane X receptor. Owing to the major role played by MRP2 in elimination of drugs and endogenous compounds, modulation of its expression may lead to adverse effects or to changes in drug pharmacokinetics.

摘要

多药耐药相关蛋白2(MRP2)是一种ATP结合盒转运蛋白,参与多种有机阴离子的胆汁、肾脏和肠道分泌,这些有机阴离子包括胆红素等内源性化合物以及药物和有毒化学物质等外源性化合物。其表达可在各种生理病理情况下受到调节,特别是在肝内胆汁淤积期间显著降低,而在某些癌组织中上调。此外,肝细胞中MRP2的水平会因糖皮质激素等激素以及利福平、苯巴比妥、利托那韦和顺铂等结构不相关的药物而发生改变。化学致癌物2-乙酰氨基芴以及oltipraz和萝卜硫素等化学预防剂也会显著增加肝实质细胞中MRP2的表达。有趣的是,大多数MRP2的化学诱导剂作用于药物代谢酶,表明这些解毒蛋白存在协同调节;所涉及的细胞机制至少部分是共同的,并且可能与孕烷X受体等核激素受体有关。由于MRP2在药物和内源性化合物消除中发挥的主要作用,其表达的调节可能会导致不良反应或药物药代动力学的变化。

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