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Biochimica et Biophysica Acta | 1988

Proton-coupled organic cation transport in renal brush-border membrane vesicles

Paul P. Sokol; Peter D. Holohan; Steven M. Grass; C R Ross

We had previously proposed that organic cations are transported across the brush-border membrane in the canine kidney by a H+ exchange (or antiport) system (Holohan, P.D. and Ross, C.R. (1981) J. Pharmacol. Exp. Ther. 216, 294-298). In the present report, we demonstrate that in brush-border membrane vesicles the transport of organic cations is chemically coupled to the countertransport of protons, by showing that the uphill or concentrative transport of a prototypic organic cation, N1-methylnicotinamide (NMN), is chemically coupled to the flow of protons down their chemical gradient. In a reciprocal manner, the concentrative transport of protons is coupled to the counterflow of organic cations down their concentration gradient. The transport of organic cations is monitored by measuring [3H]NMN while the transport of protons is monitored by measuring changes in acridine orange absorbance. The functional significance of the coupling is that a proton gradient lowers the Km and increases the Vmax for NMN transport.


Biochimica et Biophysica Acta | 1987

Cl−−HCO3− exchange in rat renal basolateral membrane vesicles

Steven M. Grassl; Peter D. Holohan; C R Ross

Pathways for HCO3- transport across the basolateral membrane were investigated using membrane vesicles isolated from rat renal cortex. The presence of Cl(-)-HCO3- exchange was assessed directly by 36Cl- tracer flux measurements and indirectly by determinations of acridine orange absorbance changes. Under 10% CO2/90% N2 the imposition of an outwardly directed HCO3- concentration gradient (pHo 6/pHi 7.5) stimulated Cl- uptake compared to Cl- uptake under 100% N2 in the presence of a pH gradient alone. Mediated exchange of Cl- for HCO3- was suggested by the HCO3- gradient-induced concentrative accumulation of intravesicular Cl-. Maneuvers designed to offset the development of ion-gradient-induced diffusion potentials had no significant effect on the magnitude of HCO3- gradient-driven Cl- uptake further suggesting chemical as opposed to electrical Cl(-)-HCO3- exchange coupling. Although basolateral membrane vesicle Cl- uptake was observed to be voltage sensitive, the DIDS insensitivity of the Cl- conductive pathway served to distinguish this mode of Cl- translocation from HCO3- gradient-driven Cl- uptake. No evidence for K+/Cl- cotransport was obtained. As determined by acridine orange absorbance measurements in the presence of an imposed pH gradient (pHo 7.5/pHi 6), a HCO3- dependent increase in the rate of intravesicular alkalinization was observed in response to an outwardly directed Cl- concentration gradient. The basolateral membrane vesicle origin of the observed Cl(-)-HCO3- exchange activity was verified by experiments performed with purified brush-border membrane vesicles. In contrast to our previous observations of the effect of Cl- on HCO3- gradient-driven Na+ uptake suggesting a basolateral membrane Na+-HCO3- for Cl- exchange mechanism, no effect of Na+ on Cl-HCO3- exchange was observed in the present study.


European Journal of Pharmacology | 1975

Reversible inhibition of (Na+ + K+)-ATPase with a cardiac glycoside☆

C R Ross; Nessah I. Pessah

The effect of a semisynthetic cardiac glycoside, Actinogen (Ay22241), on Na+ + K+ - ATPase was studied. Ay22241 was found to be as an effective inhibitor of the enzyme as ouabain, Ay22241 inhibition was a time dependent process and was completely reversible. While ouabain inhibition was also time dependent, it was only partially reversible. This reversibility with Ay22241 should make it a useful tool in studying the mode of action of cardiac glycosides.


Journal of Pharmacology and Experimental Therapeutics | 1979

Transport of organic ions in renal cortical luminal and antiluminal membrane vesicles.

J L Kinsella; P D Holohan; Ness I. Pessah; C R Ross


Journal of Pharmacology and Experimental Therapeutics | 1985

Electroneutral transport of organic cations in canine renal brush border membrane vesicles (BBMV).

P P Sokol; P D Holohan; C R Ross


Journal of Pharmacology and Experimental Therapeutics | 1988

Mechanism of ochratoxin A transport in kidney.

P P Sokol; G Ripich; P D Holohan; C R Ross


Journal of Pharmacology and Experimental Therapeutics | 1975

Binding of N1-methylnicotinamide and p-aminohippuric acid to a particulate fraction from dog kidney.

P D Holohan; Ness I. Pessah; C R Ross


Journal of Pharmacology and Experimental Therapeutics | 1987

The neurotoxins 1-methyl-4-phenylpyridinium and 1-methyl-4-phenyl-1,2,3,6- tetrahydropyridine are substrates for the organic cation transporter in renal brush border membrane vesicles.

P P Sokol; P D Holohan; C R Ross


Journal of Pharmacology and Experimental Therapeutics | 1989

Gentamicin and verapamil compete for a common transport mechanism in renal brush border membrane vesicles.

P P Sokol; K R Huiatt; P D Holohan; C R Ross


Journal of Pharmacology and Experimental Therapeutics | 1968

STUDIES OF UPTAKE AND RUNOUT OF p-AMINOHIPPURATE AND N-METHYLNICOTINAMIDE IN DOG RENAL SLICES

C R Ross; Ness I. Pessah; Alfred Farah

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Ness I. Pessah

State University of New York System

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Peter D. Holohan

State University of New York System

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D. Warkentin

State University of New York System

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Isaac N. Pessah

State University of New York System

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Nessah I. Pessah

State University of New York System

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Paul P. Sokol

State University of New York System

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Steven M. Grass

State University of New York System

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Steven M. Grassl

State University of New York System

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