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Kinetic characterization of bile salt transport by human NTCP (SLC10A1).

Authors :
Jani, Márton
Beéry, Erzsébet
Heslop, Teresa
Tóth, Beáta
Jagota, Bhavana
Kis, Emese
Kevin Park, B.
Krajcsi, Peter
Weaver, Richard J.
Source :
Toxicology in Vitro. Feb2018, Vol. 46, p189-193. 5p.
Publication Year :
2018

Abstract

The transport of bile acids facilitated by NTCP is an important factor in establishing bile flow. In this study, we examine the kinetics associated with human NTCP-dependent transport of two quantitatively important bile acids comprising the human bile acid pool, chenodeoxycholic acid and glycine-chenodeoxycholate, and secondary bile salt, 3-sulfo-glycolithocholate of potential toxicological significance. The study employed human NTCP overexpressing Chinese Hamster Ovary cells and results compared with taurocholate, a prototypical bile salt commonly used in transporter studies. GCDC and 3S-GLC but not CDCA were transported by NTCP. The efficient uptake of GCDC, TCA and 3S-GLC by NTCP enabled the determination of kinetics. GCDC displayed a lower K M (0.569 ± 0.318 μM) than TCA (6.44 ± 3.83 μM) and 3S-GLC (3.78 ± 1.17 μM). The apparent CL int value for GCDC was 20-fold greater (153 ± 53 μl/mg protein/min) than the apparent CL int for TCA (6.92 ± 4.72 μl/mg protein/min) and apparent CL int for 3S-GLC (8.05 ± 1.33 μl/mg protein/min). These kinetic results provide important complementary data on the substrate selectivity and specificity of NTCP to transport bile acids. NTCP transports GCDC with greater efficiency than TCA and has the same efficacy for 3S-GLC and TCA. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
08872333
Volume :
46
Database :
Academic Search Index
Journal :
Toxicology in Vitro
Publication Type :
Academic Journal
Accession number :
126165508
Full Text :
https://doi.org/10.1016/j.tiv.2017.10.012