Literature DB >> 1408656

Identification of sodium-dependent and sodium-independent dicarboxylate transport systems in rat liver basolateral membrane vesicles.

B Zimmerli1, B O'Neill, P J Meier.   

Abstract

The mechanisms involved in the hepatocellular uptake of Krebs-cycle intermediates were investigated in isolated basolateral (sinusoidal and lateral) rat liver plasma membrane (blLPM) vesicles. An inwardly directed Na+ gradient markedly stimulated uptake of 2-oxoglutarate and succinate into voltage- and pH-clamped blLPM vesicles. This Na(+)-dependent portion of the dicarboxylate uptake was characterized by (a) saturability with increasing substrate concentrations (Km = 6.4-10 mM; Vmax approximately 0.2 nmol min-1 mg protein-1), (b) cis-inhibition by lithium (10 mM), other Krebs-cycle dicarboxylates (1 mM) and DIDS (4,4'-diisothiocyanostilbene-2,2'-disulfonic acid; 1 mM) but not by sulphate, monocarboxylates, oxalate, acidic amino acids, bile salts and probenecid, (c) stimulation by an intravesicular negative K(+)-diffusion potential indicating electrogenic [(Na+)n greater than 2-succinate] cotransport, and (d) a pH optimum for transport between 7.0 and 7.5. In the absence of Na+, an inside alkaline pH gradient also markedly stimulated 2-oxoglutarate uptake. This pH-gradient-driven 2-oxoglutarate uptake was insensitive to lithium, but could also be inhibited by DIDS and succinate. Furthermore, saturation kinetics demonstrated Km (approximately 34 mM) and Vmax (approximately 0.8 nmol min-1 mg protein-1) values that were clearly different from those of the Na(+)-dependent uptake system. These results indicate the occurrence of two separate dicarboxylate transport systems along the sinusoidal border of hepatocytes, one being a Na(+)-dicarboxylate symporter and the other representing an anion-exchange system.

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Year:  1992        PMID: 1408656     DOI: 10.1007/bf00374220

Source DB:  PubMed          Journal:  Pflugers Arch        ISSN: 0031-6768            Impact factor:   3.657


  18 in total

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4.  Contraluminal transport systems in the proximal renal tubule involved in secretion of organic anions.

Authors:  K J Ullrich; G Rumrich
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5.  Functional hepatocyte heterogeneity. Vascular 2-oxoglutarate is almost exclusively taken up by perivenous, glutamine-synthetase-containing hepatocytes.

Authors:  B Stoll; D Hüssinger
Journal:  Eur J Biochem       Date:  1989-05-15

6.  Specificity of the transport system for tricarboxylic acid cycle intermediates in renal brush borders.

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Journal:  J Membr Biol       Date:  1980-11-15       Impact factor: 1.843

7.  Succinate and citrate transport in renal basolateral and brush-border membranes.

Authors:  S H Wright; T M Wunz
Journal:  Am J Physiol       Date:  1987-09

8.  Hepatocyte heterogeneity in uptake and metabolism of malate and related dicarboxylates in perfused rat liver.

Authors:  B Stoll; D Hüssinger
Journal:  Eur J Biochem       Date:  1991-01-01

9.  Indirect coupling to Na+ of p-aminohippuric acid uptake into rat renal basolateral membrane vesicles.

Authors:  H Shimada; B Moewes; G Burckhardt
Journal:  Am J Physiol       Date:  1987-11

10.  Structural and functional polarity of canalicular and basolateral plasma membrane vesicles isolated in high yield from rat liver.

Authors:  P J Meier; E S Sztul; A Reuben; J L Boyer
Journal:  J Cell Biol       Date:  1984-03       Impact factor: 10.539

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  2 in total

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2.  Molecular and functional analysis of SDCT2, a novel rat sodium-dependent dicarboxylate transporter.

Authors:  X Chen; H Tsukaguchi; X Z Chen; U V Berger; M A Hediger
Journal:  J Clin Invest       Date:  1999-04       Impact factor: 14.808

  2 in total

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