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首页> 外文期刊>Therapeutic Drug Monitoring >Role of P-glycoprotein in drug disposition.
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Role of P-glycoprotein in drug disposition.

机译:P-糖蛋白在药物处置中的作用。

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摘要

P-glycoprotein (Pgp), which is coded by human MDR1 (multidrug resistance) gene, is an energy-dependent efflux pump that exports its substrates out of the cell. Human Pgp is present not only in tumor cells but also in normal tissues including the kidney, liver, small and large intestine, brain, testis, and adrenal gland, and the pregnant uterus. This tissue distribution indicates that Pgp plays a significant role in excreting xenobiotics and metabolites into urine and bile and into the intestinal lumen, and in preventing their accumulation in the brain. The roles of Pgp in drug disposition include a urinary excretion mechanism in the kidney, a biliary excretion mechanism in the liver, an absorption barrier and determinant of oral bioavailability, and the blood-brain barrier that limits the accumulation of drugs in the brain. The inhibition of the transporting function of Pgp can cause clinically significant drug interactions and can also increase the penetration of drugs into the brain and the accumulation of drugs in the brain. Digoxin is a typical substrate for Pgp, which regulates the renal tubular secretion and brain distribution of digoxin. At present, potent Pgp inhibitors are being investigated in clinical trials aimed at overcoming the intrinsic or acquired multidrug resistance of human cancers. The clinical application of these Pgp inhibitors should take into consideration the physiologic function of pgp.
机译:P-糖蛋白(Pgp)由人类MDR1(多药抗性)基因编码,是一种能量依赖型外排泵,可将其底物输出到细胞外。人Pgp不仅存在于肿瘤细胞中,而且还存在于正常组织中,包括肾脏,肝脏,小肠和大肠,大脑,睾丸和肾上腺以及怀孕的子宫。这种组织分布表明,Pgp在将异生物素和代谢物排泄到尿液和胆汁以及肠腔中以及防止其在大脑中积聚方面起着重要作用。 Pgp在药物处置中的作用包括肾脏中的尿排泄机制,肝脏中的胆汁排泄机制,口服生物利用度的吸收障碍和决定因素以及限制大脑中药物蓄积的血脑屏障。 Pgp转运功能的抑制可引起临床上显着的药物相互作用,还可增加药物向大脑的渗透以及药物在脑中的积累。地高辛是Pgp的典型底物,它调节地高辛的肾小管分泌和大脑分布。目前,在临床试验中正在研究有效的Pgp抑制剂,以克服人类癌症的固有或获得性多药耐药性。这些Pgp抑制剂的临床应用应考虑pgp的生理功能。

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