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Literature DB >> 6541702

Histidyl residues at the active site of the Na/succinate co-transporter in rabbit renal brush borders.

Abstract

Mono-, dicarboxylic acid-, and D-glucose transport were measured in brush border vesicles from renal cortex after treatment with reagents known to modify terminal amino, lysyl, epsilon-amino, guanidino, serine/threonine, histidyl, tyrosyl, tryptophanyl and carboxylic residues. All three sodium-coupled co-transport systems proved to possess sulfhydryl (and maybe tryptophanyl sulfhydryl, disulfide, thioether and tyrosyl) residues but not at the substrate site or at the allosteric cavity for the Na co-ion. Histidyl groups seem to be located in the active site of the dicarboxylic transporter in that the simultaneous presence of Na and succinate protects the transporter against the histidyl specific reagent diethylpyrocarbonate. Lithium, which specifically competes for sodium sites in the dicarboxylic acid transporter, substantially blocked the protective effect of Na and succinate. Hydroxylamine specifically reversed the covalent binding of diethylpyrocarbonate to the succinate binding site. The pH dependence of the Na/succinate cotransport is consistent with an involvement of histidyl and sulfhydryl residues. We conclude that a histidyl residue is at, or is close to, the active site of the dicarboxylate transporter in renal brush border membranes.

Entities: Chemical Disease

Mesh：

Substances：

Year: 1984 PMID： 6541702 DOI： 10.1007/bf01868980

Source DB: PubMed Journal: J Membr Biol ISSN： 0022-2631 Impact factor: 1.843

53 in total

1. Crystalline pyruvate, phosphate dikinase from Bacteroides symbiosus. Modification of essential histidyl residues and bromopyruvate inactivation.

Authors: H Yoshida; H G Wood
Journal: J Biol Chem Date: 1978-11-10 Impact factor: 5.157

2. Transport of tricarboxylic acid cycle intermediates by membrane vesicles from renal brush border.

Authors: I Kippen; B Hirayama; J R Klinenberg; E M Wright
Journal: Proc Natl Acad Sci U S A Date: 1979-07 Impact factor: 11.205

3. Allosteric interactions in aspartate transcarbamylase. II. Evidence for different conformational states of the protein in the presence and absence of specific ligands.

Authors: J C Gerhart; H K Schachman
Journal: Biochemistry Date: 1968-02 Impact factor: 3.162

4. Depressant 1,2-dihydroquinolines and related derivatives.

Authors: J F Muren; A Weissman
Journal: J Med Chem Date: 1971-01 Impact factor: 7.446

5. Identification of a protein component of horse kidney brush border D-glucose transport system.

Authors: J C Poiree; R Mengual; P Sudaka
Journal: Biochem Biophys Res Commun Date: 1979-10-29 Impact factor: 3.575

6. Isolation of (a subunit of) the Na+/D-glucose cotransporter(s) of rabbit intestinal brush border membranes using monoclonal antibodies.

Authors: U M Schmidt; B Eddy; C M Fraser; J C Venter; G Semenza
Journal: FEBS Lett Date: 1983-09-19 Impact factor: 4.124

7. A rabbit erythrocyte membrane protein associated with L-lactate transport.

Authors: M L Jennings; M Adams-Lackey
Journal: J Biol Chem Date: 1982-11-10 Impact factor: 5.157

8. Comparison of the effects of certain thiol reagents on alanine transport in plasma membrane vesicles from rat liver and their use in identifying the alanine carrier.

Authors: M R Hayes; J D McGivan
Journal: Biochem J Date: 1983-08-15 Impact factor: 3.857

9. The use of a potential-sensitive cyanine dye for studying ion-dependent electrogenic renal transport of organic solutes. Uptake of L-malate and D-malate by luminal-membrane vesicles.

Authors: U Kragh-Hansen; K E Jørgensen; M I Sheikh
Journal: Biochem J Date: 1982-11-15 Impact factor: 3.857

Histidyl residues at the active site of the Na/succinate co-transporter in rabbit renal brush borders.

1. Crystalline pyruvate, phosphate dikinase from Bacteroides symbiosus. Modification of essential histidyl residues and bromopyruvate inactivation.

2. Transport of tricarboxylic acid cycle intermediates by membrane vesicles from renal brush border.

3. Allosteric interactions in aspartate transcarbamylase. II. Evidence for different conformational states of the protein in the presence and absence of specific ligands.

4. Depressant 1,2-dihydroquinolines and related derivatives.

5. Identification of a protein component of horse kidney brush border D-glucose transport system.

6. Isolation of (a subunit of) the Na+/D-glucose cotransporter(s) of rabbit intestinal brush border membranes using monoclonal antibodies.

7. A rabbit erythrocyte membrane protein associated with L-lactate transport.

8. Comparison of the effects of certain thiol reagents on alanine transport in plasma membrane vesicles from rat liver and their use in identifying the alanine carrier.

9. The use of a potential-sensitive cyanine dye for studying ion-dependent electrogenic renal transport of organic solutes. Uptake of L-malate and D-malate by luminal-membrane vesicles.

10. Pathways for carboxylic acid transport by rabbit renal brush border membrane vesicles.

1. Evidence for histidyl and carboxy groups at the active site of the human placental Na+-H+ exchanger.

2. Na+(Li+)/branched-chain amino acid cotransport in Pseudomonas aeruginosa.

3. Cysteine residues in the Na+/dicarboxylate co-transporter, NaDC-1.

4. Role for sulfur-containing groups in the Na+-Ca2+ exchange of cardiac sarcolemmal vesicles.

5. Coupling between sodium and succinate transport across renal brush border membrane vesicles.

6. Mutational analysis of histidine residues in the rabbit Na+/dicarboxylate co-transporter NaDC-1.

7. Functional characteristics of the cardiac sarcolemmal monocarboxylate transporter.

8. Folate transport in intestinal brush border membrane: involvement of essential histidine residue(s).

9. Electrophysiology of succinate transport across rabbit renal brush border membranes.

10. Inhibition of the Na+/Ca2+ antiport of heart mitochondria by diethylpyrocarbonate.