Tahara Harunobu, Kusuhara Hiroyuki, Chida Michihiro, Fuse Eiichi, Sugiyama Yuichi
Graduate School of Pharmaceutical Sciences, University of Tokyo, Hongo, Tokyo, 113-0033, Japan.
J Pharmacol Exp Ther. 2006 Mar;316(3):1187-94. doi: 10.1124/jpet.105.094052. Epub 2005 Nov 16.
The renal drug-drug interaction between famotidine (an H(2) receptor antagonist) and probenecid has not been reproduced in rats. We have proposed that this is caused by a species difference in the transport activity by human/rat organic anion transporter (OAT) 3 and the expression of organic cation transporter (OCT) 1 in the rodent kidney. Since monkey OATs (mkOATs) exhibit similar transport activities to human orthologs, it is hypothesized that in vivo studies in monkeys will allow a more precise prediction of renal drug-drug interactions in humans. Famotidine and cimetidine were efficiently taken up by mkOAT3-expressing human embryonic kidney cells (Km, 154 and 71 microM, respectively), and their uptake was strongly inhibited by probenecid (Ki, 3.0-5.7 microM). Quantification of mkOCT1 and mkOCT2 mRNAs in the monkey kidney using real-time reverse transcription-polymerase chain reaction revealed their predominant expression in the liver and kidney, respectively. Crossover studies were conducted in cynomolgus monkeys. Famotidine was given by i.v. administration, with or without probenecid. Probenecid treatment caused a 65% reduction in the renal clearance (0.426 +/- 0.079 versus 0.165 +/- 0.027 l/h/kg) and a 90% reduction in the tubular secretion clearance (0.275 +/- 0.075 versus 0.0230 +/- 0.0217 l/h/kg), whereas it had no effect on the renal clearance of cimetidine. In contrast to the species-dependent effect of probenecid, allometric scaling using animal data (rat, dog, and monkey) successfully predicted the renal and tubular secretion clearance of famotidine in humans. These results suggest that monkeys are more appropriate animal species for predicting the renal drug-drug interactions in humans.
法莫替丁(一种H₂受体拮抗剂)与丙磺舒之间的肾脏药物相互作用在大鼠中未得到重现。我们推测这是由于人/大鼠有机阴离子转运体(OAT)3的转运活性以及啮齿动物肾脏中有机阳离子转运体(OCT)1的表达存在种属差异所致。由于猴OATs(mkOATs)表现出与人类直系同源物相似的转运活性,因此推测在猴身上进行的体内研究将能更精确地预测人类的肾脏药物相互作用。法莫替丁和西咪替丁能被表达mkOAT3的人胚肾细胞有效摄取(Km分别为154和71 μM),且它们的摄取受到丙磺舒的强烈抑制(Ki为3.0 - 5.7 μM)。使用实时逆转录 - 聚合酶链反应对猴肾中的mkOCT1和mkOCT2 mRNA进行定量分析,结果显示它们分别在肝脏和肾脏中占主导性表达。在食蟹猴中进行了交叉研究。静脉注射法莫替丁,同时给予或不给予丙磺舒。丙磺舒治疗使肾脏清除率降低了65%(0.426 ± 0.079对0.165 ± 0.027 l/h/kg),使肾小管分泌清除率降低了90%(0.275 ± 0.075对0.0230 ± 0.0217 l/h/kg),而对西咪替丁的肾脏清除率没有影响。与丙磺舒的种属依赖性效应相反,使用动物数据(大鼠、狗和猴)进行的异速生长标度成功预测了人类中法莫替丁的肾脏和肾小管分泌清除率。这些结果表明,猴是预测人类肾脏药物相互作用更合适的动物种属。
