Interaction of human and rat organic anion transporter 2 with various cephalosporin antibiotics
Cephalosporin antibiotics are thought to be excreted into the urine via organic anion transporters (OATs) and OAT can mediate nephrotoxicity by cephalosporins, particularly by cephaloridine. The purpose of this study was to elucidate the interaction of human-OAT2 and rat-OAT2 with cephalosporin anti...
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th-mahidol.210332018-07-24T10:29:32Z Interaction of human and rat organic anion transporter 2 with various cephalosporin antibiotics Suparat Khamdang Michio Takeda Ellappan Babu Rie Noshiro Maristela Lika Onozato Akihiro Tojo Atsushi Enomoto Xiu Lin Huang Shinichi Narikawa Naohiko Anzai Pawinee Piyachaturawat Hitoshi Endou Kyorin University School of Medicine Mahidol University University of Tokyo Fuji Biomedix Co Ltd Pharmacology, Toxicology and Pharmaceutics Cephalosporin antibiotics are thought to be excreted into the urine via organic anion transporters (OATs) and OAT can mediate nephrotoxicity by cephalosporins, particularly by cephaloridine. The purpose of this study was to elucidate the interaction of human-OAT2 and rat-OAT2 with cephalosporin antibiotics using proximal tubule cells stably expressing human-OAT2 and rat-OAT2. Human-OAT2 is localized to the basolateral side of the proximal tubule, whereas rat-OAT2 is localized to the apical side of the proximal tubule. Cephalosporins tested were cephalothin, cefoperazone, cefazolin, ceftriaxone, cephaloridine, cefotaxime, cefadroxil and cefamandole. These cephalosporins dose-dependently inhibited organic anion uptake mediated by human-OAT2 and rat-OAT2. There was no species difference observed for the effects of OAT2 with cephalosporins between human and rat transporters. Kinetic analysis revealed that the inhibitory effects for human-OAT2 were competitive. Cephaloridine significantly decreased the viability of cells stably expressing human-OAT2, human-OAT1, human-OAT3 and human-OAT4. The decreased viability of cells stably expressing human-OAT1, human-OAT3 and human-OAT4 but not human-OAT2 was reversed by probenecid. In conclusion, human-OAT2 interacts with cephalosporins, and thus, human-OAT2 may mediate the uptake of cephalosporins on the basolateral side of the proximal tubule. The interaction of human-OAT2 with cephalosporins was the weakest among the basolateral human-OATs tested. In addition, it is suggested that human-OATs mediate cephaloridine-induced nephrotoxicity. © 2003 Elsevier Science B.V. All rights reserved. 2018-07-24T03:29:32Z 2018-07-24T03:29:32Z 2003-03-28 Article European Journal of Pharmacology. Vol.465, No.1-2 (2003), 1-7 10.1016/S0014-2999(03)01381-5 00142999 2-s2.0-10744219672 https://repository.li.mahidol.ac.th/handle/123456789/21033 Mahidol University SCOPUS https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=10744219672&origin=inward |
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Pharmacology, Toxicology and Pharmaceutics Suparat Khamdang Michio Takeda Ellappan Babu Rie Noshiro Maristela Lika Onozato Akihiro Tojo Atsushi Enomoto Xiu Lin Huang Shinichi Narikawa Naohiko Anzai Pawinee Piyachaturawat Hitoshi Endou Interaction of human and rat organic anion transporter 2 with various cephalosporin antibiotics |
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Cephalosporin antibiotics are thought to be excreted into the urine via organic anion transporters (OATs) and OAT can mediate nephrotoxicity by cephalosporins, particularly by cephaloridine. The purpose of this study was to elucidate the interaction of human-OAT2 and rat-OAT2 with cephalosporin antibiotics using proximal tubule cells stably expressing human-OAT2 and rat-OAT2. Human-OAT2 is localized to the basolateral side of the proximal tubule, whereas rat-OAT2 is localized to the apical side of the proximal tubule. Cephalosporins tested were cephalothin, cefoperazone, cefazolin, ceftriaxone, cephaloridine, cefotaxime, cefadroxil and cefamandole. These cephalosporins dose-dependently inhibited organic anion uptake mediated by human-OAT2 and rat-OAT2. There was no species difference observed for the effects of OAT2 with cephalosporins between human and rat transporters. Kinetic analysis revealed that the inhibitory effects for human-OAT2 were competitive. Cephaloridine significantly decreased the viability of cells stably expressing human-OAT2, human-OAT1, human-OAT3 and human-OAT4. The decreased viability of cells stably expressing human-OAT1, human-OAT3 and human-OAT4 but not human-OAT2 was reversed by probenecid. In conclusion, human-OAT2 interacts with cephalosporins, and thus, human-OAT2 may mediate the uptake of cephalosporins on the basolateral side of the proximal tubule. The interaction of human-OAT2 with cephalosporins was the weakest among the basolateral human-OATs tested. In addition, it is suggested that human-OATs mediate cephaloridine-induced nephrotoxicity. © 2003 Elsevier Science B.V. All rights reserved. |
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Kyorin University School of Medicine |
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Kyorin University School of Medicine Suparat Khamdang Michio Takeda Ellappan Babu Rie Noshiro Maristela Lika Onozato Akihiro Tojo Atsushi Enomoto Xiu Lin Huang Shinichi Narikawa Naohiko Anzai Pawinee Piyachaturawat Hitoshi Endou |
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Article |
author |
Suparat Khamdang Michio Takeda Ellappan Babu Rie Noshiro Maristela Lika Onozato Akihiro Tojo Atsushi Enomoto Xiu Lin Huang Shinichi Narikawa Naohiko Anzai Pawinee Piyachaturawat Hitoshi Endou |
author_sort |
Suparat Khamdang |
title |
Interaction of human and rat organic anion transporter 2 with various cephalosporin antibiotics |
title_short |
Interaction of human and rat organic anion transporter 2 with various cephalosporin antibiotics |
title_full |
Interaction of human and rat organic anion transporter 2 with various cephalosporin antibiotics |
title_fullStr |
Interaction of human and rat organic anion transporter 2 with various cephalosporin antibiotics |
title_full_unstemmed |
Interaction of human and rat organic anion transporter 2 with various cephalosporin antibiotics |
title_sort |
interaction of human and rat organic anion transporter 2 with various cephalosporin antibiotics |
publishDate |
2018 |
url |
https://repository.li.mahidol.ac.th/handle/123456789/21033 |
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1763496347204321280 |