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Vol. 289, Issue 1, 66-71, April 1999
-Lactam Antibiotic Ceftibuten in Rat
Intestinal Brush-Border Membrane
Department of Pharmacy, Hokkaido University Hospital, School of
Medicine, Hokkaido University, Kita-ku, Sapporo, Japan
To elucidate the transport characteristics of the
H+/dipeptide carrier that recognizes the orally active
-lactam antibiotic ceftibuten, the uptake behaviors were compared of
ceftibuten and Gly-Sar by rat intestinal brush-border membrane
vesicles. The results show that 1) both the uptake of ceftibuten and
that of Gly-Sar were dependent on an inwardly directed H+
gradient; 2) anionic compounds such as hippurylphenyllactic acid competitively inhibited ceftibuten uptake in the presence of
H+ gradient, whereas this anion did not inhibit Gly-Sar
uptake; and 3) the carrier-mediated uptake of ceftibuten did not
disappear even in the presence of 20 mM Gly-Sar. The results provide an evidence that several transporters with different features are potentially responsible for the uptake of
-lactam antibiotics into
the intestinal cells. It is suggested that the dianionic
-lactam
antibiotics that carry a net negative charge such as ceftibuten use
multiple H+-dependent transport systems for absorption.
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