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三磷酸腺苷结合盒(ABC)药物转运蛋白在外周血细胞中的表达:对生理学和药物治疗的意义。

Expression of adenosine triphosphate-binding cassette (ABC) drug transporters in peripheral blood cells: relevance for physiology and pharmacotherapy.

作者信息

Köck Kathleen, Grube Markus, Jedlitschky Gabriele, Oevermann Lena, Siegmund Werner, Ritter Christoph A, Kroemer Heyo K

机构信息

Department of Pharmacology, Research Center of Pharmacology and Experimental Therapeutics, Ernst Moritz Arndt University, Greifswald, Germany.

出版信息

Clin Pharmacokinet. 2007;46(6):449-70. doi: 10.2165/00003088-200746060-00001.

Abstract

Adenosine triphosphate-binding cassette (ABC)-type transport proteins were initially described for their ability to reduce intracellular concentrations of anticancer compounds, thereby conferring drug resistance. In recent years, expression of this type of proteins has also been reported in numerous cell types under physiological conditions; here, these transporters are often reported to alter systemic and local drug disposition (e.g. in the brain or the gastrointestinal tract). In this context, peripheral blood cells have also been found to express several ABC-type transporters. While erythrocytes mainly express multidrug resistance protein (MRP) 1, MRP4 and MRP5, which are discussed with regard to their involvement in glutathione homeostasis (MRP1) and in the efflux of cyclic nucleotides (MRP4 and MRP5), leukocytes also express P-glycoprotein and breast cancer resistance protein. In the latter cell types, the main function of efflux transporters may be protection against toxins, as these cells demonstrate a very high turnover rate. In platelets, only two ABC transporters have been described so far. Besides MRP1, platelets express relatively high amounts of MRP4 not only in the plasma membrane but also in the membrane of dense granules, suggesting relevance for mediator storage. In addition to its physiological function, ABC transporter expression in these structures can be of pharmacological relevance since all systemic drugs reach their targets via circulation, thereby enabling interaction of the therapeutic agent with peripheral blood cells. Moreover, both intended effects and unwanted side effects occur in peripheral blood cells, and intracellular micropharmacokinetics can be affected by these transport proteins. The present review summarises the data available on expression of ABC transport proteins in peripheral blood cells.

摘要

三磷酸腺苷结合盒(ABC)型转运蛋白最初因其降低细胞内抗癌化合物浓度从而赋予耐药性的能力而被描述。近年来,在生理条件下,这种类型的蛋白也在多种细胞类型中被报道有表达;在此情况下,这些转运蛋白常被报道会改变全身和局部的药物处置(如在大脑或胃肠道中)。在这种背景下,外周血细胞也被发现表达几种ABC型转运蛋白。红细胞主要表达多药耐药蛋白(MRP)1、MRP4和MRP5,它们分别在谷胱甘肽稳态(MRP1)以及环核苷酸外排(MRP4和MRP5)方面受到讨论,白细胞也表达P-糖蛋白和乳腺癌耐药蛋白。在后者这些细胞类型中,外排转运蛋白的主要功能可能是抵御毒素保护细胞,因为这些细胞具有非常高的更新率。在血小板中,到目前为止仅描述了两种ABC转运蛋白。除了MRP1,血小板不仅在质膜而且在致密颗粒膜中都表达相对大量的MRP4,这表明其与介质储存有关。除了其生理功能外,这些结构中ABC转运蛋白的表达还可能具有药理学相关性,因为所有全身药物都通过循环到达其靶点,从而使治疗药物能够与外周血细胞相互作用。此外,外周血细胞中会出现预期效果和不良副作用,并且细胞内微药代动力学可能会受到这些转运蛋白的影响。本综述总结了关于外周血细胞中ABC转运蛋白表达的现有数据。

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