Literature DB >> 16541252

The solute carrier family SLC10: more than a family of bile acid transporters regarding function and phylogenetic relationships.

J Geyer1, T Wilke, E Petzinger.   

Abstract

The solute carrier family 10 (SLC10) comprises two sodium-dependent bile acid transporters, i.e. the Na(+)/taurocholate cotransporting polypeptide (NTCP; SLC10A1) and the apical sodium-dependent bile acid transporter (ASBT; SLC10A2). These carriers are essentially involved in the maintenance of the enterohepatic circulation of bile acids mediating the first step of active bile acid transport through the membrane barriers in the liver (NTCP) and intestine (ASBT). Recently, four new members of the SLC10 family were described and referred to as P3 (SLC10A3), P4 (SLC10A4), P5 (SLC10A5) and sodium-dependent organic anion transporter (SOAT; SLC10A6). Experimental data supporting carrier function of P3, P4, and P5 is currently not available. However, as demonstrated for SOAT, not all members of the SLC10 family are bile acid transporters. SOAT specifically transports steroid sulfates such as oestrone-3-sulfate and dehydroepiandrosterone sulfate in a sodium-dependent manner, and is considered to play an important role for the cellular delivery of these prohormones in testes, placenta, adrenal gland and probably other peripheral tissues. ASBT and SOAT are the most homologous members of the SLC10 family, with high sequence similarity ( approximately 70%) and almost identical gene structures. Phylogenetic analyses of the SLC10 family revealed that ASBT and SOAT genes emerged from a common ancestor gene. Structure-activity relationships of NTCP, ASBT and SOAT are discussed at the amino acid sequence level. Based on the high structural homology between ASBT and SOAT, pharmacological inhibitors of the ASBT, which are currently being tested in clinical trials for cholesterol-lowering therapy, should be evaluated for their cross-reactivity with SOAT.

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Year:  2006        PMID: 16541252     DOI: 10.1007/s00210-006-0043-8

Source DB:  PubMed          Journal:  Naunyn Schmiedebergs Arch Pharmacol        ISSN: 0028-1298            Impact factor:   3.000


  111 in total

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Authors:  H Jung
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4.  Discovery of potent, nonsystemic apical sodium-codependent bile acid transporter inhibitors (Part 1).

Authors:  Samuel J Tremont; Len F Lee; Horng-Chih Huang; Bradley T Keller; Shyamal C Banerjee; Scott R Both; Andrew J Carpenter; Ching-Cheng Wang; Danny J Garland; Wei Huang; Claude Jones; Kevin J Koeller; Steve A Kolodziej; James Li; Robert E Manning; Matthew W Mahoney; Raymond E Miller; Deborah A Mischke; Nigam P Rath; Theresa Fletcher; Emily J Reinhard; Michael B Tollefson; William F Vernier; Grace M Wagner; Steve R Rapp; Judy Beaudry; Kevin Glenn; Karen Regina; Joe R Schuh; Mark E Smith; Jay S Trivedi; David B Reitz
Journal:  J Med Chem       Date:  2005-09-08       Impact factor: 7.446

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Journal:  J Lipid Res       Date:  1993-10       Impact factor: 5.922

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Journal:  Hepatology       Date:  1999-07       Impact factor: 17.425

7.  Modulation by drugs of human hepatic sodium-dependent bile acid transporter (sodium taurocholate cotransporting polypeptide) activity.

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Journal:  J Pharmacol Exp Ther       Date:  1999-12       Impact factor: 4.030

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Journal:  Semin Liver Dis       Date:  2000       Impact factor: 6.115

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Journal:  Hepatology       Date:  1997-12       Impact factor: 17.425

10.  Expression and characterization of a functional rat liver Na+ bile acid cotransport system in COS-7 cells.

Authors:  J L Boyer; O C Ng; M Ananthanarayanan; A F Hofmann; C D Schteingart; B Hagenbuch; B Stieger; P J Meier
Journal:  Am J Physiol       Date:  1994-03
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Review 6.  Drug uptake systems in liver and kidney: a historic perspective.

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7.  Identification of zebrafish steroid sulfatase and comparative analysis of the enzymatic properties with human steroid sulfatase.

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Review 8.  Bile acid transporters in health and disease.

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