Abstract

We studied unidirectional [14C]HCO3- efflux from human resealed red cell ghosts with 1 mM acetazolamide under self-exchange conditions at pH = pH(i = o) 7.4-9.0 and 0-38 degrees C by means of the Millipore-Swinnex and continuous flow tube filtering techniques. 14CO2 loss from cells to efflux medium and further to the atmosphere was insignificant. [14C]HCO3- efflux was determined at pH 7.8, 38 degrees C under symmetric variation of the HCO3- concentrations (C(i = o)), and asymmetric conditions: C(i) varied, C(o) constant, or C(o) varied, C(i) constant. MM-fit, Jeff = Jmaxeff x C x (C + K1/2)-1, used to describe the concentration dependence of Jeff,o when only C(o) varied, yields at C(i) = 50 mM: K1/2o = 3.8 mMJ, Jmaxeff.o = 20 nmol cm-2 s-1; at C(i) = 165 mM: K1/2o = 10 mM, Jmaxeff.o = 32 nmol cm-2 s-1. When C(i) varied, noncompetitive self inhibition by HCO3- binding (inhibitor constant K1) to an intracellular site was included (MS-fit). Under conditions of (a) symmetry: C(i = o) = 9-600 mM, K1/2s = 173 mM, K1 = 172 mM, and Jmaxeff,s = 120 nmol cm-2 s-1, (b) asymmetry: C(o) = 50 mM, K1/2i = 116 mM, K1 = 136 mM, and Jmaxeff,i = 92 nmol cm-2 s-1. All flux parameters accord with the ping-pong model for anion exchange. The data for C(i) < 200 mM also fit well to the MM equation, but K1/2 and Jmaxeff are different from the MS-fit and are inconsistent with the ping-pong model. Thus, self-inhibition (MS-fit) must be included even at low concentrations. As at 0 degree C, the system is asymmetric: 8-10 times more unloaded transport sites face inward than outward when C(i = o). Jeff,s was not mono-exponentially dependent on temperature at 0-38 degrees C, indicating that the transmembrane anion transport is controlled by several rate constants with different temperature dependencies. Jeff,s was not significantly affected by increasing pH(i = o) from 7.4 to 7.8, but it decreased by 50% when pH was raised to 9.0.

Highlights

  • Red blood cells play an important role in transport of metabolic gases in the human body

  • One important step in the removal of carbon dioxide from oxygenconsuming tissues to the lungs is the exchange of bicarbonate for chloride across the erythrocyte membrane, referred to as the "Hamburger Shift," that involves the transmembrane protein, called band 3 based on its electrophoretic characteristics (Fairbanks et al, 1971); capnophorin, i.e., "smoke carrier" (Wieth and Bjerrum, 1983) based on the physiological role of the transport protein in the removal of CO 2, the "smoke" that results from metabolism; or AE1 to emphasize its membership in a genetically related family of anion exchangers (Kopito, 1990)

  • By comparing chloride exchange flux at body temperature with the flux determined as net current of anions (Hunter, 1977) it became clear that anion exchange is a highly electroneutral process and that net transport of anions, possibly performed by capnophorin, is about five orders of magnitude slower than the exchange transport

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Summary

Introduction

Red blood cells play an important role in transport of metabolic gases in the human body. One important step in the removal of carbon dioxide from oxygenconsuming tissues to the lungs is the exchange of bicarbonate for chloride across the erythrocyte membrane, referred to as the "Hamburger Shift," that involves the transmembrane protein, called band 3 based on its electrophoretic characteristics (Fairbanks et al, 1971); capnophorin, i.e., "smoke carrier" (Wieth and Bjerrum, 1983) based on the physiological role of the transport protein in the removal of CO 2, the "smoke" that results from metabolism; or AE1 to emphasize its membership in a genetically related family of anion exchangers (Kopito, 1990). By exploiting the high time resolution of the continuous flow tube technique, Brahm (1977) extended the temperature range for studies of chloride transport up to body temperature. By comparing chloride exchange flux at body temperature with the flux determined as net current of anions (Hunter, 1977) it became clear that anion exchange is a highly electroneutral process and that net transport of anions, possibly performed by capnophorin, is about five orders of magnitude slower than the exchange transport

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