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Vol. 290, Issue 1, 388-392, July 1999
Department of Pharmacy, Kyoto University Hospital, Faculty of
Medicine, Kyoto University, Sakyo-ku, Kyoto, Japan
Transport characteristics of diphenhydramine, an antihistamine, were
studied in cultured human intestinal Caco-2 cell monolayers to
elucidate the mechanisms of its intestinal absorption. Diphenhydramine accumulation in the monolayers increased rapidly and was influenced by
extracellular pH (pH 7.4 > 6.5 > 5.5). Diphenhydramine
uptake was temperature dependent, saturable, and not potential
sensitive. Kinetic analysis revealed that the apparent
Km values were constant (0.8-1.0 mM) in all
pH conditions tested, whereas Vmax values decreased at the lower pH. The initial uptake of diphenhydramine was
competitively inhibited by another antihistamine, chlorpheniramine, with a Ki value of 1.3 mM. On the other
hand, cimetidine and tetraethylammonium, typical substrates for the
renal organic cation transport system, had no effect. Moreover,
biological amines and neurotransmitters, such as histamine, dopamine,
serotonin, and choline, also had no effect on the diphenhydramine
accumulation. Finally, diphenhydramine uptake was stimulated by
preloading monolayers with chlorpheniramine (trans-stimulation effect). These findings indicate that
diphenhydramine transport in Caco-2 cells is mediated by a specific
transport system. This pH-dependent transport system may contribute to
the intestinal absorption of diphenhydramine.
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