Bile Acid Uptake via the Human Apical Sodium-Bile Acid Cotransporter Is Electrogenic

doi:10.1074/jbc.273.52.34691

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Bile Acid Uptake via the Human Apical Sodium-Bile Acid Cotransporter Is Electrogenic

Steven A. Weinman^§, Michael W. Carruth, and Paul A. Dawson

From the Department of Physiology and Biophysics and ^§ Department of Internal Medicine, University of Texas Medical Branch, Galveston, Texas 77555 and the Department of Internal Medicine, Wake Forest University School of Medicine, Wake Forest University, Winston-Salem, North Carolina 27157

Intestinal absorption of bile acids depends on a sodium-bile acid cotransport protein in the apical membrane of the ilealepithelial cell. Transport is Na⁺-dependent, but the Na⁺-bile acid stoichiometry and electrogenicity of transport arenot known. Studies in whole intestine, isolated cells, and ilealmembrane vesicles have been unable to resolve this issue becausetransport currents are small and can be obscured by other ionicconductances and transport proteins present in these membranes.In this study, the human apical sodium-bile acid transporter wasexpressed in stably transfected Chinese hamster ovary cells thatlack other bile acid transporters. The Na⁺-dependent transport of a fluorescent bile acid analog, chenodeoxycholyl-N $epsilon$ -nitrobenzoxadiazol-lysine,was monitored by fluorescence microscopy in single, voltage-clampedcells. Bile acid movement was bidirectional and voltage-dependentwith negative intracellular voltage-stimulating influx. A 3-foldreduction in extracellular Na⁺ produced a negative 52 mV shift of the flux-voltage relationship,consistent with a 2:1 Na⁺:bile acid coupling stoichiometry. No Na⁺- or voltage-dependent uptake was observed in nontransfected Chinesehamster ovary cells. These results indicate that the cotransportof bile acids and Na⁺ by human apical sodium-bile acid transporter is electrogenicand bidirectional and is best explained by a 2:1 Na⁺:bile acid coupling stoichiometry. These results suggest thatmembrane potential may regulate bile acid transport rates underphysiological and pathophysiologicalconditions.

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