Literature DB >> 3631279

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

S H Wright, T M Wunz.   

Abstract

Properties of the Na-dependent transport of succinate and citrate were determined in brush-border and basolateral membrane vesicles (BBMV and BLMV, respectively) isolated from the rabbit renal cortex. As has been shown in previous studies, the initial rate of uptake of these substrates into BBMV was markedly stimulated (50- to 150-fold) by an inwardly directed Na gradient. In BLMV, uptake of 5 microM succinate was also stimulated (150-fold) by a Na gradient, and the profile of the time course of accumulation was qualitatively and quantitatively different from that in BBMV. In contrast, basolateral uptake of 2 microM citrate was stimulated only one- to fivefold by a Na gradient. The external pH had little effect on uptake of succinate into BBMV or BLMV, or on uptake of citrate into BLMV. Uptake of citrate into BBMV, however, was stimulated 10-fold by reducing external pH from 8 to 5.5. Valinomycin-induced K diffusion potentials stimulated succinate uptake into BBMV and BLMV, suggesting that Na-coupled succinate transport across both membranes is electrogenic. The Jmax and apparent Kt for uptake into BBMV were much greater than those in BLMV (90 vs. 5 nmol X mg-1 X min-1 and 0.61 vs. 0.01 mM, respectively). Inhibition of succinate uptake by several polycarboxylates suggested that the BLMV transporter had a higher apparent affinity for dicarboxylates than for tricarboxylates, compared with the BBMV transporter. We conclude that BLMV possess a low-capacity, high-affinity Na-dependent transport pathway showing a high degree of specificity for dicarboxylic, rather than tricarboxylic, acids.

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Year:  1987        PMID: 3631279     DOI: 10.1152/ajprenal.1987.253.3.F432

Source DB:  PubMed          Journal:  Am J Physiol        ISSN: 0002-9513


  19 in total

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2.  Localization of the calcium-regulated citrate transport process in proximal tubule cells.

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3.  Tumor microenvironment promotes dicarboxylic acid carrier-mediated transport of succinate to fuel prostate cancer mitochondria.

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4.  A choline transporter in renal brush-border membrane vesicles: energetics and structural specificity.

Authors:  S H Wright; T M Wunz; T P Wunz
Journal:  J Membr Biol       Date:  1992-02       Impact factor: 1.843

5.  Expression of sodium-dependent dicarboxylate transporter 1 (NaDC1/SLC13A2) in normal and neoplastic human kidney.

Authors:  Hyun-Wook Lee; Mary E Handlogten; Gunars Osis; William L Clapp; Dara N Wakefield; Jill W Verlander; I David Weiner
Journal:  Am J Physiol Renal Physiol       Date:  2016-12-07

Review 6.  Sodium-coupled dicarboxylate and citrate transporters from the SLC13 family.

Authors:  Ana M Pajor
Journal:  Pflugers Arch       Date:  2013-10-10       Impact factor: 3.657

7.  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

8.  Competitive inhibition of p-aminohippurate transport by quinapril in rabbit renal basolateral membrane vesicles.

Authors:  W Akarawut; D E Smith
Journal:  J Pharmacokinet Biopharm       Date:  1998-06

9.  Modulation by anions of p-aminohippurate transport in bovine renal basolateral membrane vesicles.

Authors:  C Schmitt; G Burckhardt
Journal:  Pflugers Arch       Date:  1993-11       Impact factor: 3.657

10.  p-Aminohippurate/2-oxoglutarate exchange in bovine renal brush-border and basolateral membrane vesicles.

Authors:  C Schmitt; G Burckhardt
Journal:  Pflugers Arch       Date:  1993-05       Impact factor: 3.657

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