Taurocholate transport by hepatic and intestinal bile acid transporters is independent of FIC1 overexpression in Madin-Darby canine kidney cells.

[benign recurrent intrahepatic cholestasis]

Mutations in the human familial intrahepatic cholestasis gene , FIC 1 , result in progressive familial intrahepatic cholestasis type 1 in children and benign recurrent intrahepatic cholestasis . The present study was performed to determine whether FIC 1 transports bile acids and /or influences the activity of apical bile acid transporters .The apical secretion assay utilized transfected Madin-Darby canine kidney (MDCK ) cells , which stably express the bile acid uptake protein , Na +/taurocholate co -transporting polypeptide (NTCP ). These cells were then transiently transfected with FIC 1 and /or the bile salt export pump (BSEP ) and were grown on Transwell filters to form a polarized monolayer . [(3 )H ]Taurocholate was added to the basal medium and the taurocholate secretion was measured in the apical medium . A second assay , apical uptake assays , utilized polarized MDCK-II cells , which were transiently transfected with FIC 1 , FIC 1 mutants and /or the apical sodium-dependent bile acid transporter (ASBT ). [(3 )H ]Taurocholate was added to the apical media and intracellular uptake of taurocholate was measured .Apical secretion assays : FIC 1 expression in MDCK /NTCP cells had no effect on taurocholate secretion compared to controls . In contrast , apical secretion of taurocholate in BSEP-transfected cells was approximately twofold higher than in non-transfected MDCK /NTCP cells (P < 0 .01 ). The BSEP-mediated secretion was unaffected by co -transfection with FIC 1 . Apical uptake assays : taurocholate uptake in ASBT expressing cells was 6 .5 -fold higher than in controls and was unaffected by co -transfection of cells with FIC 1 or FIC 1 mutants .These results indicate that FIC 1 does not transport taurocholate and , when overexpressed in MDCK cells , had no effect on the function of BSEP or ABST .