TRANSPORT MECHANISM OF CEPHALEXIN IN ISOLATED HEPATOCYTES

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概要

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• By using isolated rat hepatocytes, the mechanism of uptake of a zwitterionic β-lactam antibiotic, cephalexin, was clarified. The uptake followed the combination of saturable carrier-mediated and nonsaturable first-order rate processes. The kinetic parameters were estimated as follows (mean±SD) : maximum uptake rate (V_<max>), 2.28±0.24 nmol/min/mg of protein ; Michaelis constant (K_t), 6.28±0.31 mM and first-order rate constant (k_d), 0.11±0.012 nmol/min/mg of protein/mM. There was no inhibitory effect by amino acids, dipeptides or organic cations, whereas an organic anion, probenecid, markedly inhibited the hepatic uptake of cephalexin. Several β-lactam antibiotics including zwitterionic and anionic derivatives inhibited cephalexin uptake significantly. The inhibition kinetics revealed that benzylpenicillin and the stereo-isomer l-cephalexin competitively inhibited cephalexin uptake. Furthermore, the efflux of cephalexin from the cells was stimulated by adding benzylpenicillin in the extracellular medium. These results demonstrated that all β-lactam antibiotics have a common transport system with an organic anion such as probenecid, irrespective of their ionic charges, though a cationic charge on the molecule is less advantageous for being recognized by the carrier system.

• 公益社団法人日本薬学会の論文

著者

• Tsuji Akira

  Faculty Of Pharmaceutical Sciences Kanazawa University

• Tsuji Akira

  富山化学工業綜合研究所

• Tamai I

  Tokyo Univ. Sci. Tokyo Jpn

• Tamai Ikumi

  Meiji Seika Kaisha Ltd. Pharmaceutical Research Center:department Of Surgery Kawasaki City Ida Hospi

• Tamai Ikumi

  Faculty Of Pharmaceutical Sciences Tokyo University Of Science

• Tamai Ikumi

  Department Of Pharmaceutics Faculty Of Pharmaceutical Sciences Kanazawa University

• Tamai Ikumi

  Faculty Of Pharmaceutical Sciences And Hospital Pharmacy Kanazawa University

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