Importance of uncharged polar residues and proline in the proximal two-thirds (Pro(107)–Ser(128)) of the highly conserved region of mouse ileal Na(+)-dependent bile acid transporter, Slc10a2, in transport activity and cellular expression

BACKGROUND: SLC10A2-mediated reabsorption of bile acids at the distal end of the ileum is the first step in enterohepatic circulation. Because bile acids act not only as detergents but also as signaling molecules in lipid metabolism and energy production, SLC10A2 is important as the key transporter...

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Autores principales: Saeki, Tohru, Sato, Kosuke, Ito, Shiho, Ikeda, Keisuke, Kanamoto, Ryuhei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3570448/
https://www.ncbi.nlm.nih.gov/pubmed/23374508
http://dx.doi.org/10.1186/1472-6793-13-4
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author Saeki, Tohru
Sato, Kosuke
Ito, Shiho
Ikeda, Keisuke
Kanamoto, Ryuhei
author_facet Saeki, Tohru
Sato, Kosuke
Ito, Shiho
Ikeda, Keisuke
Kanamoto, Ryuhei
author_sort Saeki, Tohru
collection PubMed
description BACKGROUND: SLC10A2-mediated reabsorption of bile acids at the distal end of the ileum is the first step in enterohepatic circulation. Because bile acids act not only as detergents but also as signaling molecules in lipid metabolism and energy production, SLC10A2 is important as the key transporter for understanding the in vivo kinetics of bile acids. SLC10A family members and the homologous genes of various species share a highly conserved region corresponding to Gly(104)–Pro(142) of SLC10A2. The functional importance of this region has not been fully elucidated. RESULTS: To elucidate the functional importance of this region, we previously performed mutational analysis of the uncharged polar residues and proline in the distal one-third (Thr(130)–Pro(142)) of the highly conserved region in mouse Slc10a2. In this study, proline and uncharged polar residues in the remaining two-thirds of this region in mouse Slc10a2 were subjected to mutational analysis, and taurocholic acid uptake and cell surface localization were examined. Cell surface localization of Slc10a2 is necessary for bile acid absorption. Mutants in which Asp or Leu were substituted for Pro(107) (P107N or P107L) were abundantly expressed, but their cell surface localization was impaired. The S126A mutant was completely impaired in cellular expression. The T110A and S128A mutants exhibited remarkably enhanced membrane expression. The S112A mutant was properly expressed at the cell surface but transport activity was completely lost. Replacement of Tyr(117) with various amino acids resulted in reduced transport activity. The degree of reduction roughly depended on the van der Waals volume of the side chains. CONCLUSIONS: The functional importance of proline and uncharged polar residues in the highly conserved region of mouse Slc10a2 was determined. This information will contribute to the design of bile acid-conjugated prodrugs for efficient drug delivery or SLC10A2 inhibitors for hypercholesterolemia treatment.
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spelling pubmed-35704482013-02-13 Importance of uncharged polar residues and proline in the proximal two-thirds (Pro(107)–Ser(128)) of the highly conserved region of mouse ileal Na(+)-dependent bile acid transporter, Slc10a2, in transport activity and cellular expression Saeki, Tohru Sato, Kosuke Ito, Shiho Ikeda, Keisuke Kanamoto, Ryuhei BMC Physiol Research Article BACKGROUND: SLC10A2-mediated reabsorption of bile acids at the distal end of the ileum is the first step in enterohepatic circulation. Because bile acids act not only as detergents but also as signaling molecules in lipid metabolism and energy production, SLC10A2 is important as the key transporter for understanding the in vivo kinetics of bile acids. SLC10A family members and the homologous genes of various species share a highly conserved region corresponding to Gly(104)–Pro(142) of SLC10A2. The functional importance of this region has not been fully elucidated. RESULTS: To elucidate the functional importance of this region, we previously performed mutational analysis of the uncharged polar residues and proline in the distal one-third (Thr(130)–Pro(142)) of the highly conserved region in mouse Slc10a2. In this study, proline and uncharged polar residues in the remaining two-thirds of this region in mouse Slc10a2 were subjected to mutational analysis, and taurocholic acid uptake and cell surface localization were examined. Cell surface localization of Slc10a2 is necessary for bile acid absorption. Mutants in which Asp or Leu were substituted for Pro(107) (P107N or P107L) were abundantly expressed, but their cell surface localization was impaired. The S126A mutant was completely impaired in cellular expression. The T110A and S128A mutants exhibited remarkably enhanced membrane expression. The S112A mutant was properly expressed at the cell surface but transport activity was completely lost. Replacement of Tyr(117) with various amino acids resulted in reduced transport activity. The degree of reduction roughly depended on the van der Waals volume of the side chains. CONCLUSIONS: The functional importance of proline and uncharged polar residues in the highly conserved region of mouse Slc10a2 was determined. This information will contribute to the design of bile acid-conjugated prodrugs for efficient drug delivery or SLC10A2 inhibitors for hypercholesterolemia treatment. BioMed Central 2013-02-04 /pmc/articles/PMC3570448/ /pubmed/23374508 http://dx.doi.org/10.1186/1472-6793-13-4 Text en Copyright ©2013 Saeki et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Saeki, Tohru
Sato, Kosuke
Ito, Shiho
Ikeda, Keisuke
Kanamoto, Ryuhei
Importance of uncharged polar residues and proline in the proximal two-thirds (Pro(107)–Ser(128)) of the highly conserved region of mouse ileal Na(+)-dependent bile acid transporter, Slc10a2, in transport activity and cellular expression
title Importance of uncharged polar residues and proline in the proximal two-thirds (Pro(107)–Ser(128)) of the highly conserved region of mouse ileal Na(+)-dependent bile acid transporter, Slc10a2, in transport activity and cellular expression
title_full Importance of uncharged polar residues and proline in the proximal two-thirds (Pro(107)–Ser(128)) of the highly conserved region of mouse ileal Na(+)-dependent bile acid transporter, Slc10a2, in transport activity and cellular expression
title_fullStr Importance of uncharged polar residues and proline in the proximal two-thirds (Pro(107)–Ser(128)) of the highly conserved region of mouse ileal Na(+)-dependent bile acid transporter, Slc10a2, in transport activity and cellular expression
title_full_unstemmed Importance of uncharged polar residues and proline in the proximal two-thirds (Pro(107)–Ser(128)) of the highly conserved region of mouse ileal Na(+)-dependent bile acid transporter, Slc10a2, in transport activity and cellular expression
title_short Importance of uncharged polar residues and proline in the proximal two-thirds (Pro(107)–Ser(128)) of the highly conserved region of mouse ileal Na(+)-dependent bile acid transporter, Slc10a2, in transport activity and cellular expression
title_sort importance of uncharged polar residues and proline in the proximal two-thirds (pro(107)–ser(128)) of the highly conserved region of mouse ileal na(+)-dependent bile acid transporter, slc10a2, in transport activity and cellular expression
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3570448/
https://www.ncbi.nlm.nih.gov/pubmed/23374508
http://dx.doi.org/10.1186/1472-6793-13-4
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