Metformin is a superior substrate for renal organic cation transporter OCT2 rather than hepatic OCT1

N Kimura, S Masuda, Y Tanihara, H Ueo… - Drug metabolism and …, 2005 - jstage.jst.go.jp
N Kimura, S Masuda, Y Tanihara, H Ueo, M Okuda, T Katsura, K Inui
Drug metabolism and pharmacokinetics, 2005jstage.jst.go.jp
Although metformin, a cationic agent for type II diabetes, shows its pharmacological eŠect in
the liver, the drug is mainly eliminated into urine. The tissue selectivity based on the function
of drug transporters is unclear. In the present study, the transport of metformin was examined
using HEK293 cells transiently transfected with ˆve human renal organic ion transporter
cDNAs. Human OCT1 and OCT2, but not OAT1, OAT3 or OCT2-A, stimulated the uptake. A
kinetic analysis of metformin transport demonstrated that the amount of plasmid cDNA for …
Summary
Although metformin, a cationic agent for type II diabetes, shows its pharmacological eŠect in the liver, the drug is mainly eliminated into urine. The tissue selectivity based on the function of drug transporters is unclear. In the present study, the transport of metformin was examined using HEK293 cells transiently transfected with ˆve human renal organic ion transporter cDNAs. Human OCT1 and OCT2, but not OAT1, OAT3 or OCT2-A, stimulated the uptake. A kinetic analysis of metformin transport demonstrated that the amount of plasmid cDNA for transfection was also important parameter to the quantitative elucidation of functional characteristics of transporters, and both human and rat OCT2 had about a 10-and 100-fold greater capacity to transport metformin than did OCT1, respectively. In male rats, the mRNA expression level of rOCT2 in the whole kidneys was 8-fold greater than that of rOCT1 in the whole liver. The in vivo distribution of metformin in rats revealed that the expression level of renal OCT2 was a key factor in the control of the concentrative accumulation of metformin in the kidney. These ˆndings suggest that metformin is a superior substrate for renal OCT2 rather than hepatic OCT1, and renal OCT2 plays a dominant role for metformin pharmacokinetics.
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