Your search keyword '"Knauf PA"' showing total 30 results

1. Inhibition of Na+/H+ exchanger enhances low pH-induced L-selectin shedding and beta2-integrin surface expression in human neutrophils.

Author

Kaba NK, Schultz J, Law FY, Lefort CT, Martel-Gallegos G, Kim M, Waugh RE, Arreola J, and Knauf PA

Subjects

Amiloride pharmacology, Ammonium Chloride metabolism, CD11b Antigen metabolism, Cell Membrane immunology, Cell Membrane metabolism, Guanidines pharmacology, Humans, Hydrogen-Ion Concentration, Lactic Acid metabolism, Macrophage-1 Antigen metabolism, Metalloproteases antagonists & inhibitors, Metalloproteases metabolism, Neutrophils immunology, Neutrophils metabolism, Protease Inhibitors pharmacology, Protein Kinase Inhibitors pharmacology, Reperfusion Injury immunology, Reperfusion Injury metabolism, Reperfusion Injury prevention & control, Sodium-Hydrogen Exchangers metabolism, Sulfones pharmacology, Time Factors, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors, p38 Mitogen-Activated Protein Kinases metabolism, Amiloride analogs & derivatives, CD18 Antigens metabolism, Cell Membrane drug effects, L-Selectin metabolism, Neutrophils drug effects, Sodium-Hydrogen Exchangers antagonists & inhibitors

Abstract

Ischemia-reperfusion injury is a common pathological occurrence causing tissue damage in heart attack and stroke. Entrapment of neutrophils in the vasculature during ischemic events has been implicated in this process. In this study, we examine the effects that lactacidosis and consequent reductions in intracellular pH (pH(i)) have on surface expression of adhesion molecules on neutrophils. When human neutrophils were exposed to pH 6 lactate, there was a marked decrease in surface L-selectin (CD62L) levels, and the decrease was significantly enhanced by inclusion of Na(+)/H(+) exchanger (NHE) inhibitor 5-(N,N-hexamethylene)amiloride (HMA). Similar effects were observed when pH(i) was reduced while maintaining normal extracellular pH, by using an NH(4)Cl prepulse followed by washes and incubation in pH 7.4 buffer containing NHE inhibitors [HMA, cariporide, or 5-(N,N-dimethyl)amiloride (DMA)]. The amount of L-selectin shedding induced by different concentrations of NH(4)Cl in the prepulse correlated with the level of intracellular acidification with an apparent pK of 6.3. In contrast, beta(2)-integrin (CD11b and CD18) was only slightly upregulated in the low-pH(i) condition and was enhanced by NHE inhibition to a much lesser extent. L-selectin shedding was prevented by treating human neutrophils with inhibitors of extracellular metalloproteases (RO-31-9790 and KD-IX-73-4) or with inhibitors of intracellular signaling via p38 MAP kinase (SB-203580 and SB-239063), implying a transmembrane effect of pH(i). Taken together, these data suggest that the ability of NHE inhibitors such as HMA to reduce ischemia-reperfusion injury may be related to the nearly complete removal of L-selectin from the neutrophil surface.

Published

2008

2. Mechanical shedding of L-selectin from the neutrophil surface during rolling on sialyl Lewis x under flow.

Author

Lee D, Schultz JB, Knauf PA, and King MR

Subjects

Humans, Ligands, Neutrophils cytology, Shear Strength, p38 Mitogen-Activated Protein Kinases metabolism, L-Selectin metabolism, Leukocyte Rolling physiology, Lewis X Antigen chemistry, Lewis X Antigen metabolism, N-Acetylneuraminic Acid chemistry, N-Acetylneuraminic Acid metabolism, Neutrophils physiology

Abstract

The interaction of L-selectin expressed on leukocytes with endothelial cells leads to capture and rolling and is critical for the recruitment of leukocytes into sites of inflammation. It is known that leukocyte activation by chemoattractants, the change of osmotic pressure in cell media, or cross-linking of L-selectin all result in rapid shedding of L-selectin. Here we present a novel mechanism for surface cleavage of L-selectin on neutrophils during rolling on a sialyl Lewis x-coated surface that involves mechanical force. Flow cytometry and rolling of neutrophils labeled with Qdot(R)-L-selectin antibodies in an in vitro flow chamber showed that the mechanical shedding of L-selectin occurs during rolling and depends on the amount of shear applied. In addition, the mechanical L-selectin shedding causes an increase in cell rolling velocity with rolling duration, suggesting a gradual loss of L-selectin and is mediated by p38 mitogen-activated protein kinase activation. Thus, these data show that mechanical force induces the cleavage of L-selectin from the neutrophil surface during rolling and therefore decreases the adhesion of cells to a ligand-presenting surface in flow.

Published

2007

3. A novel immobilization method for single protein spFRET studies.

Author

Pal P, Lesoine JF, Lieb MA, Novotny L, and Knauf PA

Subjects

Adsorption, Bacterial Proteins immunology, Coated Materials, Biocompatible analysis, DNA-Binding Proteins immunology, Protein Binding, Anion Exchange Protein 1, Erythrocyte analysis, Bacterial Proteins chemistry, Biotin chemistry, Coated Materials, Biocompatible chemistry, DNA-Binding Proteins chemistry, Fluorescence Resonance Energy Transfer methods, Membrane Transport Proteins analysis, Polyethylene Glycols chemistry, Streptavidin chemistry

Abstract

We have developed a new method for immobilization of single proteins by utilizing streptavidin-biotin and protein L-antibody interactions on glass coverslips coated with polyethylene glycol. The method is particularly well suited for single-molecule fluorescence studies. A monomeric, detergent-solubilized bacterial transport protein, GlpT, and the dimeric cytoplasmic region of a mammalian transporter, cdAE1, were immobilized by our method with a high degree of specificity. The fluorescence from single molecules attached to the immobilized proteins was detected with a high signal/noise ratio. Single-pair fluorescence resonance energy transfer (spFRET) measurements on cdAE1 dimers indicate that the structure of the protein is not compromised and provide evidence that the cdAE1 protein can exist in at least two conformations under physiological conditions.

Published

2005

4. Substrate-dependent reversal of anion transport site orientation in the human red blood cell anion-exchange protein, AE1.

Author

Knauf PA, Law FY, Leung TW, Gehret AU, and Perez ML

Subjects

Anions, Bicarbonates metabolism, Biological Transport, Chlorides metabolism, Humans, Anion Exchange Protein 1, Erythrocyte metabolism, Erythrocytes metabolism

Abstract

The tightly coupled, one-for-one exchange of anions mediated by the human red blood cell AE1 anion-exchange protein involves a ping-pong mechanism, in which AE1 alternates between a state with the anion-binding site facing inward toward the cytoplasm (Ei) and a state with the site facing outward toward the external medium (Eo). The conformational shift (Ei <--> Eo) is only permitted when a suitable substrate such as Cl(-) or HCO(3)(-) (B(-)) is bound. With no anions bound, or with Cl(-) bound, far more AE1 molecules are in the inward-facing than the outward-facing forms (Ei Eo, ECli EClo). We have constructed a model for CI(-)-B(-) exchange based on Cl(-)-Cl(-) and B(-)-B(-) exchange data, and have used it to predict the heteroexchange flux under extremely asymmetric conditions, with either all Cl(-) inside and all B(-) outside (Cli-Bo) or vice versa (Bi-Clo). The experimental values of the ratio of the exchange rate for Bi-Clo to that for Cli-Bo are only compatible with the model if the asymmetry of bicarbonate-loaded sites (A(B) = EBo/EBi) > 10, the opposite of the asymmetry for unloaded or Cl-loaded sites. Furthermore, the Eo form has a higher affinity for HCO(3)(-) than for Cl(-), whereas the Ei form has a higher affinity for Cl(-). The fact that this "passive" system exhibits changes in substrate selectivity with site orientation ("sidedness"), a characteristic usually associated with energy-coupled "active" pumps, suggests that changes in affinity with changes in sidedness are a more general property of transport proteins than previously thought.

Published

2002

5. Hypotonicity induces L-selectin shedding in human neutrophils.

Author

Kaba NK and Knauf PA

Subjects

CD18 Antigens metabolism, Humans, Metalloendopeptidases metabolism, Microcirculation immunology, Tumor Necrosis Factor-alpha metabolism, Hypotonic Solutions pharmacology, L-Selectin metabolism, Neutrophils metabolism, Water-Electrolyte Balance physiology

Abstract

Expression levels of adhesion molecules on neutrophils are affected under various conditions, including ischemia, possibly because of associated increases in cell volume. We examined the effects of cell swelling in hypotonic media on the level of L-selectin (CD62L) and beta(2)-integrin (CD18) on human neutrophils. In hypotonic media, neutrophils shed L-selectin. The shedding was greatly reduced by 30 microM RO31-9790, the metalloprotease (sheddase) inhibitor. Hypotonicity-induced L-selectin shedding was also time and tonicity dependent. Decreasing tonicity caused increased shedding. In 0.6x medium (0.6x the normal tonicity of 300 mosmol/kgH(2)O), shedding increased over a 2-h period, after which >70% of the neutrophils had lost L-selectin. In contrast to L-selectin, the level of beta(2)-integrin on the neutrophil surface was not significantly affected. Thus L-selectin shedding, which occurs on neutrophil activation and is usually accompanied by beta(2)-integrin upregulation, was selectively induced by hypotonicity without a corresponding effect on beta(2)-integrin.

Published

2001

6. The noncompetitive inhibitor WW781 senses changes in erythrocyte anion exchanger (AE1) transport site conformation and substrate binding.

Author

Knauf PA, Raha NM, and Spinelli LJ

Subjects

Barbiturates pharmacology, Binding Sites physiology, Coloring Agents pharmacology, Humans, Isoxazoles pharmacology, Kinetics, Protein Conformation, Structure-Activity Relationship, Anion Exchange Protein 1, Erythrocyte chemistry, Antiporters physiology, Erythrocyte Membrane physiology

Abstract

WW781 binds reversibly to red blood cell AE1 and inhibits anion exchange by a two-step mechanism, in which an initial complex (complex 1) is rapidly formed, and then there is a slower equilibration to form a second complex (complex 2) with a lower free energy. According to the ping-pong kinetic model, AE1 can exist in forms with the anion transport site facing either inward or outward, and the transition between these forms is greatly facilitated by binding of a transportable substrate such as Cl(-). Both the rapid initial binding of WW781 and the formation of complex 2 are strongly affected by the conformation of AE1, such that the forms with the transport site facing outward have higher affinity than those with the transport site facing inward. In addition, binding of Cl(-) seems to raise the free energy of complex 2 relative to complex 1, thereby reducing the equilibrium binding affinity, but Cl(-) does not compete directly with WW781. The WW781 binding site, therefore, reveals a part of the AE1 structure that is sensitive to Cl(-) binding and to transport site orientation, in addition to the disulfonic stilbene binding site. The relationship of the inhibitory potency of WW781 under different conditions to the affinities for the different forms of AE1 provides information on the possible asymmetric distributions of unloaded and Cl(-)-loaded transport sites that are consistent with the ping-pong model, and supports the conclusion from flux and nuclear magnetic resonance data that both the unloaded and Cl(-)-loaded sites are very asymmetrically distributed, with far more sites facing the cytoplasm than the outside medium. This asymmetry, together with the ability of WW781 to recruit toward the forms with outward-facing sites, implies that WW781 may be useful for changing the conformation of AE1 in studies of structure-function relationships.

Published

2000

7. The asymmetry of chloride transport at 38 degrees C in human red blood cell membranes.

Author

Knauf PA, Gasbjerg PK, and Brahm J

Subjects

Anion Exchange Protein 1, Erythrocyte metabolism, Binding, Competitive, Biological Transport drug effects, Chlorides antagonists & inhibitors, Flufenamic Acid metabolism, Flufenamic Acid pharmacology, Humans, Kinetics, Models, Biological, Chlorides pharmacokinetics, Erythrocyte Membrane metabolism, Temperature

Abstract

Band 3-mediated Cl- exchange in human red blood cells and resealed ghosts was measured at 38 degrees C by the continuous flow tube method. When external Cl- concentration, C(o), is varied with constant internal Cl- concentration, C(i), the flux fits a simple Michaelis-Menten saturation curve (MM fit), with K1/2o = 3.8 +/- 0.4 mM. When the Cl- concentration is varied simultaneously at both sides of the membrane in resealed ghosts (C(i) = C(o) = C(i = o)), the flux rises toward a flat maximum between 200 and 450 mM Cl-, and then decreases at very high C(i = o). An MM fit to the data with C(i = o) < 500 mM gives K1/2s of 106 +/- 13 mM; fits including modifier site inhibition (MS fit) give an over threefold higher K1/2s. Despite this uncertainty, the intrinsic asymmetry of unloaded transport sites, A (defined as E(o)/E(i) with C(i) = C(o), where E(i) is the fraction of unloaded inward-facing sites and E(o) is the fraction of unloaded outward-facing sites), calculated from K1/2s and K1/2o, ranges only from 0.046 to 0.107. A new method, which uses the initial slope of a plot of Cl- flux versus C(i = o), gives A values of 0.023 to 0.038. Flufenamic acid (FA) inhibits Cl- exchange by binding to an external site different from the transport site. At 38 degrees C, FA binds 24-36 times more tightly to E(o) than to E(i). Estimates of A from FA inhibitory potency range from 0.01 to 0.05. All methods, including bicarbonate data from the preceding paper, indicate that at 38 degrees C, like 0 degree C, far more band 3 molecules are in the E(i) than in the E(o) form. The agreement of various methods supports the ping-pong model for anion exchange, and demonstrates that the intrinsic asymmetry is very slightly, if at all, affected by temperature.

Published

1996

8. Kinetics of bicarbonate transport in human red blood cell membranes at body temperature.

Author

Gasbjerg PK, Knauf PA, and Brahm J

Subjects

4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid pharmacology, Bicarbonates antagonists & inhibitors, Biological Transport drug effects, Humans, Hydrogen-Ion Concentration, Kinetics, Models, Biological, Temperature, Bicarbonates pharmacokinetics, Body Temperature, Erythrocyte Membrane metabolism

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.

Published

1996

9. Effects of external pH on binding of external sulfate, 4.4-dinitro-stilbene-2,2'-disulfonate (DNDS), and chloride to the band 3 anion exchange protein.

Author

Liu SQ, Ries E, and Knauf PA

Subjects

Amino Acids analysis, Anion Exchange Protein 1, Erythrocyte chemistry, Anion Exchange Protein 1, Erythrocyte drug effects, Binding, Competitive physiology, Chlorides pharmacology, Cross-Linking Reagents pharmacology, Humans, Hydrogen-Ion Concentration, Iodides metabolism, Iodides pharmacology, Kinetics, Stilbenes pharmacology, Succinimides pharmacology, Sulfates metabolism, Sulfates pharmacology, Anion Exchange Protein 1, Erythrocyte metabolism, Chlorides metabolism, Stilbenes metabolism

Abstract

A model in which two positively-charged titratable sites enhance the affinity for anionic substrates can explain the increase in external iodide dissociation constant (K(O)(I)) with increasing pH(O) (Liu, S. J., F.-Y. Law, and P.A. Knauf. 1996.f Gen.Physiol. 107:271-291). If sulfate binds to the same external site as I-, this model predicts that the SO(4)= dissociation constant (K(O)(S)) should also increase. The data at pH 0 8.5 to 10 fit this prediction, and the pK for the titration is not significantly different from that (pKc) for the low-pK group that affects K(O)(1). The dissociation constant for the apparently competitive inhibitor, DNDS (4,4-dinitrostilbene-2,2'-disulfonate), also increases greatly as pH(O) increases. Particularly at high pH(O), a noncompetitive inhibition by DNDS is also evident. Increasing pH(O) from 7.2 to 11.2 increases the competitive dissociation constant by 700-fold, but the noncompetitive is only increased 20-fold. The pK values for these effects are similar to pKc for K(O)(1), as expected if DNDS binds near the external transport site, but it seems likely that additional titratable groups also affect DNDS binding. The apparent affinity for external Cl- is also affected by pH(O), in a manner similar to that observed for I-. Pretreatment with the amino-selective reagent, bis-sulfosuccinimidyl suberate (BSSS), decreases the apparent Cl- affinity at pH 8.5, but two titrations are still evident, the first (lower) of which decreases the apparent C- affinity, and the second of which surprisingly increases it. Thus, the BSSS-reactive amino groups (probably Lys-539 and Lys-851) do not seem to be involved in the titrations that affect Cl- affinity. In general, the data support the concept that a positively charged amino group (or groups), together with a guanidino group, plays an important role in the binding of substrates and inhibitors at or near the external transport site.

Published

1996

10. Detection of Cl- binding to band 3 by double-quantum-filtered 35Cl nuclear magnetic resonance.

Author

Liu D, Knauf PA, and Kennedy SD

Subjects

Anion Exchange Protein 1, Erythrocyte chemistry, Anion Exchange Protein 1, Erythrocyte drug effects, Binding Sites, Biophysical Phenomena, Biophysics, Chlorides chemistry, Chlorine, Eosine Yellowish-(YS) analogs & derivatives, Eosine Yellowish-(YS) pharmacology, Humans, In Vitro Techniques, Ion Transport drug effects, Stilbenes pharmacology, Anion Exchange Protein 1, Erythrocyte metabolism, Chlorides metabolism, Magnetic Resonance Spectroscopy methods

Abstract

We have applied double-quantum-filtered (DQF) NMR of 35Cl to study binding of Cl- to external sites on intact red blood cells, including the outward-facing anion transport sites of band 3, an integral membrane protein. A DQF 35Cl NMR signal was observed in cell suspensions containing 150 mM KCl, but the DQF signal can be totally eliminated by adding 500 microM 4,4'-dinitrostilbene-2,2'-disulfonate (DNDS), an inhibitor that interferes with Cl- binding to the band 3 transport site. Therefore, it seems that only the binding of Cl- to transport sites of band 3 can give rise to a 35Cl DQF signal from red blood cell suspensions. In accordance with this concept, analysis of the single quantum free induction decay (FID) revealed that signals from buffer and DNDS-treated cells were fitted with a single exponential function, whereas the FID signals of untreated control cells were biexponential. The DQF signal remained after the cells were treated with eosin-5-maleimide (EM), a noncompetitive inhibitor of chloride exchange. This result supports previous reports that EM does not block the external chloride binding site. The band 3-dependent DQF signal is shown to be caused at least in part by nonisotropic motions of Cl- in the transport site, resulting in incompletely averaged quadrupolar couplings.

Published

1996

11. Effects of external pH on substrate binding and on the inward chloride translocation rate constant of band 3.

Author

Liu SQ, Law FY, and Knauf PA

Subjects

Allosteric Regulation, Amino Acids chemistry, Amino Acids metabolism, Anion Exchange Protein 1, Erythrocyte chemistry, Anticoagulants pharmacology, Binding, Competitive physiology, Cations metabolism, Citric Acid pharmacology, Humans, Hydrogen-Ion Concentration, Iodides pharmacology, Kinetics, Titrimetry, Anion Exchange Protein 1, Erythrocyte metabolism, Chlorides metabolism, Models, Chemical

Abstract

To test the hypothesis that amino acid residues in band 3 with titratable positive charges play a role in the binding of anions to the outside-facing transport site, we measured the effects of changing external pH (pH(O)) on the dissociation constant for binding of external iodide to the transport site, K(O)(I). K(O)(I) increased with increasing pH(O), and a significant increase was seen even at pH(O) values as low as 9.9. The dependence of K(O)(I) on pH(O) can be explained by a model with one titratable site with pK 9.5 +/- 0.2 (probably lysine), which increases anion affinity for the external transport site when it is in the positively charged form. A more complex model, analogous to one recently proposed by Bjerrum (1992), with two titratable sites, one with pK 9.3 +/- 0.3 (probably lysine) and another with pK > 11 (probably arginine), gives a slightly better fit to the data. Thus, titratable positively charged residues seem to be functionally important for the binding of substrate anions to the outward-facing anion transport site. In addition, analysis of Dixon plot slopes for L inhibition of Cl- exchange at different pH 0 values, coupled with the assumption that pH(O) has parallel effects on external I- and Cl- binding, indicates that k', the rate-constant for inward translocation of the complex of Cl- with the extracellular transport site, decreases with increasing pH(O). The data are compatible with a model in which titration of the pK 9.3 residue decreases k to 14 +/- 10% of its value at neutral pH(O). This result, however, together with Bjerrum's (1992) observation that the maximum flux J(M)) increases 1.6-fold when this residue is deprotonated, makes quantitative predictions that raise significant questions about the adequacy of the two titratable site ping-pong model or the assumptions used in analyzing the data.

Published

1996

12. 35Cl nuclear magnetic resonance line broadening shows that eosin-5-maleimide does not block the external anion access channel of band 3.

Author

Liu D, Kennedy SD, and Knauf PA

Subjects

Anion Exchange Protein 1, Erythrocyte chemistry, Binding Sites, Binding, Competitive, Biophysical Phenomena, Biophysics, Chlorides chemistry, Eosine Yellowish-(YS) pharmacology, Hematocrit, Hemolysis, Humans, In Vitro Techniques, Iodides chemistry, Ion Channels chemistry, Ion Exchange, Magnetic Resonance Spectroscopy, Models, Chemical, Stilbenes pharmacology, Anion Exchange Protein 1, Erythrocyte drug effects, Eosine Yellowish-(YS) analogs & derivatives, Fluorescent Dyes pharmacology, Ion Channels drug effects

Abstract

It has been suggested that Lys-430 of band 3, with which eosin-5-maleimide (EM) reacts, is located in the external channel through which anions gain access to the external transport site, and that EM inhibits anion exchange by blocking this channel. To test this, we have used 35Cl nuclear magnetic resonance (NMR) to measure Cl- binding to the external transport site in control and EM-treated human red blood cells. Intact cells were used rather than ghosts, because in this case all line broadening (LB) results from binding to external sites. In an NMR spectrometer with a 9.4-T magnetic field, red blood cells at 50% concentration (v/v) in 150 mM Cl- medium at 3 degrees C caused 19.0 +/- 1.2 Hz LB. Of this, 7.9 +/- 0.7 Hz was due to Cl- binding to the high affinity band 3 transport sites, because it was prevented by an apparently competitive inhibitor of anion exchange, 4,4'-dinitrostilbene-2,2'-disulfonate (DNDS). The LB was not due to hemoglobin released from the cells, as little LB remained in the supernatant after cells were removed by centrifugation. Saturable Cl- binding remained in EM-treated cells, although the binding was no longer DNDS-sensitive, because EM prevents binding of DNDS. The lower limit for the rate at which Cl- goes from the binding site to the external medium is 2.15 x 10(5) s-1 for control cells and 1.10 x 10(5) s-1 for EM-treated cells, far higher than the Cl- translocation rate at 3 degrees C (about 400 s-1). Thus, EM does not inhibit Cl- exchange by blocking the external access channel. EM may therefore be useful for fixing band 3 in one conformation for studies of Cl- binding to the external transport site.

Published

1995

13. A novel method to differentiate between ping-pong and simultaneous exchange kinetics and its application to the anion exchanger of the HL60 cell.

Author

Restrepo D, Cronise BL, Snyder RB, and Knauf PA

Subjects

Bicarbonates metabolism, Binding Sites, Extracellular Space metabolism, Humans, Intracellular Fluid metabolism, Iodobenzoates, Ion Transport drug effects, Kinetics, Models, Biological, Salicylates pharmacology, Tumor Cells, Cultured drug effects, Chlorides metabolism, Tumor Cells, Cultured metabolism

Abstract

We have developed a new test to differentiate between ping-pong and simultaneous mechanisms for tightly coupled anion exchange. This test requires the use of a dead-end reversible noncompetitive inhibitor. As an example, we have applied the test to the anion exchanger of the HL60 cell using the salicylic acid derivative 3,5-diiodosalicylic acid (DIS), which reversibly inhibits HL60 cell Cl/Cl exchange. The concentration of DIS that causes 50% inhibition (ID50) increased only slightly as either intra- or extracellular chloride was increased, indicating that DIS inhibits HL60 anion exchange in a noncompetitive manner. In agreement with this observation, plots of the slope of the Dixon plot as a function of 1/[Clo] or 1/[Cli] were fit with straight lines with nonzero intercepts, indicating that DIS does not compete with either of the substrates ([Clo] and [Cli]). The secondary Dixon slope test is based on the fact that, for a dead-end inhibitor such as DIS, the slope of the Dixon plot slope vs. 1/[Cli] (secondary Dixon slope or SDS) is independent of extracellular Cl when the exchange mechanism follows ping-pong kinetics. Similarly, the SDS calculated from a plot as a function of 1/[Clo] is also independent of intracellular Cl for a ping-pong exchanger. In contrast to this prediction, we found that for DIS inhibition of Cl/Cl exchange in HL60 cells the slope of the Dixon plot slope vs. 1/[Cli] decreased by a factor of 2.5-fold when [Clo] was increased from 1 to 11 mM (P < 0.0001). This change in the SDS rules out ping-pong kinetics, but is consistent with a simultaneous model of Cl/Cl exchange in which there are extra- and intracellular anion binding sites, both of which must be occupied by suitable anions in order to allow simultaneous exchange of the ions.

Published

1992

14. Use of niflumic acid to determine the nature of the asymmetry of the human erythrocyte anion exchange system.

Author

Knauf PA and Mann NA

Subjects

Anion Transport Proteins, Chlorides pharmacology, Humans, Hydrogen-Ion Concentration, Membrane Potentials, Models, Biological, Tissue Distribution, Carrier Proteins metabolism, Nicotinic Acids, Niflumic Acid

Abstract

Niflumic acid is a noncompetitive inhibitor of chloride exchange, which binds to a site different from the transport or modifier sites. When the internal Cl- concentration is raised, at constant extracellular Cl-, the inhibitory potency of niflumic acid increases. This effect cannot be attributed to changes in membrane potential, but rather it suggests that niflumic acid binds to the anion exchange protein band 3 only when the transport site faces outward. When the chloride gradient is reversed, with Clo greater than Cli , the inhibitory potency of niflumic acid decreases greatly, which indicates that the affinity of niflumic acid for band 3 with the transport site facing inward is almost 50 times less than when the transport site faces outward. Experiments in which Cli = Clo show no significant change in the inhibition by niflumic acid when Cl- is lowered from 150 to 10 mM. These data suggest that the intrinsic dissociation constants for Cl- at the two sides of the membrane are nearly equal. Thus, the chloride-loaded transport sites have an asymmetric orientation like that of the unloaded transport sites, with approximately 15 times more sites facing the inside than the outside. The asymmetry reflects an approximately 1.5 kcal/mol free energy difference between the inward-facing and outward-facing chloride-loaded forms of band 3. High concentrations of chloride (with Cli = Clo), which partially saturate the modifier site, have no effect on niflumic acid inhibition, which indicates that chloride binds equally well to the modifier site regardless of the orientation of the transport site.

Published

1984

15. pH homeostasis in promyelocytic leukemic HL60 cells.

Author

Restrepo D, Kozody DJ, Spinelli LJ, and Knauf PA

Subjects

4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid, 4-Acetamido-4'-isothiocyanatostilbene-2,2'-disulfonic Acid analogs & derivatives, 4-Acetamido-4'-isothiocyanatostilbene-2,2'-disulfonic Acid pharmacology, Carrier Proteins metabolism, Cell Line, Chloride-Bicarbonate Antiporters, Dimethyl Sulfoxide pharmacology, Homeostasis, Humans, Membrane Potentials, Pentachlorophenol pharmacology, Sodium-Hydrogen Exchangers, Tetraethylammonium Compounds pharmacology, Hydrogen-Ion Concentration, Leukemia, Promyelocytic, Acute physiopathology

Abstract

By measuring the membrane potential using the influx of the lipophilic cation tetraphenylphosphonium and intracellular pH using 2,7-biscarboxy-ethyl-5(6)-carboxyfluorescein and the distribution of the weak acid 5,5-dimethyl-2,4-oxazolidinedione, we have determined that intracellular pH is 0.9-1.1 pH units above electrochemical equilibrium in undifferentiated HL60 cells, indicating that these cells actively extrude proton equivalents. The Na/H exchanger is not the system responsible for keeping the pH above the electrochemical equilibrium, since adding inhibitors of this transport system (dimethylamiloride and ethylisopropylamiloride) or removing the extracellular sodium has no effect on intracellular pH. In contrast, the addition of the Cl/HCO3 exchange inhibitors H2 4,4'-diisothiocyanostilbene-2,2'-disulfonate (DIDS) or pentachlorophenol (PCP) causes a drop in intracellular pH, and the removal of extracellular chloride in the presence of bicarbonate leads to a large intracellular alkalinization, which indicates a role for the anion exchanger in pH homeostasis in these cells. In addition, we find that the intracellular chloride concentration is about one order of magnitude above electrochemical equilibrium. We conclude that an H2DIDS and PCP inhibitable system, probably the Cl/HCO3 exchanger, is at least partially responsible for keeping intracellular pH above electrochemical equilibrium in HL60 cells under resting conditions. We also find no change in intracellular pH when cells differentiate along the granulocytic pathway (having been induced by the addition of dimethylsulfoxide or of retinoic acid), which indicates that changes in intracellular pH are not causally related to cell differentiation.

Published

1988

16. Mechanism of the increase in cation permeability of human erythrocytes in low-chloride media. Involvement of the anion transport protein capnophorin.

Author

Jones GS and Knauf PA

Subjects

4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid, 4-Acetamido-4'-isothiocyanatostilbene-2,2'-disulfonic Acid analogs & derivatives, 4-Acetamido-4'-isothiocyanatostilbene-2,2'-disulfonic Acid pharmacology, Humans, In Vitro Techniques, Nystatin pharmacology, Potassium metabolism, Rubidium metabolism, Sodium metabolism, Anion Exchange Protein 1, Erythrocyte physiology, Carrier Proteins physiology, Cell Membrane Permeability drug effects, Chlorides physiology, Erythrocyte Membrane metabolism

Abstract

When human erythrocytes are suspended in low-Cl- media (with sucrose replacing Cl-), there is a large increase in both the net efflux and permeability of K+. A substantial portion (greater than 70% with Cl- less than 12.5 mM) of this K+ efflux is inhibited by the anion exchange inhibitor DIDS (4,4'-diisothiocyanostilbene-2,2'-disulfonic acid). This inhibition cannot be explained as an effect of DIDS on net Cl- permeability (Pcl) and membrane potential, but rather represents a direct effect on the K+ permeability. When cells are reacted with DIDS for different times, the inhibition of K+ efflux parallels that of Cl- exchange, which strongly indicates that the band 3 anion exchange protein (capnophorin) mediates the net K+ flux. Since a noncompetitive inhibitor of anion exchange, niflumic acid, has no effect on net K+ efflux, the net K+ flow does not seem to involve the band 3 conformational change that mediates anion exchange. The data suggest that in low-Cl- media, the anion selectivity of capnophorin decreases so that it can act as a very low-conductivity channel for cations. Na+ and Rb+, as well as K+, can utilize this pathway.

Published

1985

17. Effects of the transport site conformation on the binding of external NAP-taurine to the human erythrocyte anion exchange system. Evidence for intrinsic asymmetry.

Author

Knauf PA, Law FY, Tarshis T, and Furuya W

Subjects

Anion Transport Proteins, Biological Transport, Chlorides pharmacology, Humans, Hydrogen-Ion Concentration, Membrane Potentials, Models, Biological, Taurine metabolism, Tissue Distribution, Anions metabolism, Carrier Proteins metabolism, Taurine analogs & derivatives

Abstract

External N-(4-azido-2-nitrophenyl)-2-aminoethylsulfonate (NAP-taurine) inhibits human red cell chloride exchange by binding to a site that is distinct from the chloride transport site. Increases in the intracellular chloride concentration (at constant external chloride) cause an increase in the inhibitory potency of external NAP-taurine. This effect is not due to the changes in pH or membrane potential that usually accompany a chloride gradient, since even when these changes are reversed or eliminated the inhibitory potency remains high. According to the ping-pong model for anion exchange, such transmembrane effects of intracellular chloride on external NAP-taurine can be explained if NAP-taurine only binds to its site when the transport site is in the outward-facing (Eo or EClo ) form. Since NAP-taurine prevents the conformational change from EClo to ECli , it must lock the system in the outward-facing form. NAP-taurine can therefore be used just like the competitive inhibitor H2DIDS (4,4'-diisothiocyano-1,2- diphenylethane -2,2'-disulfonic acid) to monitor the fraction of transport sites that face outward. A quantitative analysis of the effects of chloride gradients on the inhibitory potency of NAP-taurine and H2DIDS reveals that the transport system is intrinsically asymmetric, such that when Cli = Clo, most of the unloaded transport sites face the cytoplasmic side of the membrane.

Published

1984

18. Relationship of net chloride flow across the human erythrocyte membrane to the anion exchange mechanism.

Author

Knauf PA, Law FY, and Marchant PJ

Subjects

Adult, Biomechanical Phenomena, Bromides physiology, Chlorides pharmacology, Chlorides physiology, Fluorides physiology, Humans, Hydrogen-Ion Concentration, Iodides physiology, Models, Biological, Taurine analogs & derivatives, Taurine pharmacology, Water metabolism, Anions metabolism, Chlorides metabolism, Erythrocyte Membrane metabolism, Erythrocytes metabolism

Abstract

The parallel effects of the anion transport inhibitor DIDS (4,4'-diisothiocyanostilbene-2,2'-disulfonate) on net chloride flow and on chloride exchange suggest that a major portion of net chloride flow takes place through the anion exchange system. The "slippage" model postulates that the rate of net anion flow is determined by the movement of the unloaded anion transport site across the membrane. Both the halide selectivity of net anion flow and the dependence of net chloride flux on chloride concentration over the range of 75 to 300 mM are inconsistent with the slippage model. Models in which the divalent form of the anion exchange carrier or water pores mediate net anion flow are also inconsistent with the data. The observations that net chloride flux increases with chloride concentration and that the DIDS-sensitive component tends to saturate suggest a model in which net anion flow involves "transit" of anions through the diffusion barriers in series with the transport site, without any change in transport site conformation such as normally occurs during the anion exchange process. This model is successful in predicting that the anion exchange inhibitor NAP-taurine, which binds to the modifier site and inhibits the conformational change, has less effect on net chloride flow than on chloride exchange.

Published

1983

19. Relationship of the decreases in protein synthesis and intracellular Na+ during friend murine erythroleukemic cell differentiation.

Author

Lannigan DA, Knauf PA, and Macara IG

Subjects

Amino Acids metabolism, Animals, Cell Differentiation drug effects, Cell Line, Cycloheximide pharmacology, Dimethyl Sulfoxide pharmacology, Hydrogen-Ion Concentration, Kinetics, Leukemia, Erythroblastic, Acute pathology, Leukemia, Experimental pathology, Mice, Onium Compounds metabolism, Organophosphorus Compounds metabolism, Leukemia, Erythroblastic, Acute metabolism, Leukemia, Experimental metabolism, Neoplasm Proteins biosynthesis, Sodium metabolism

Abstract

The earliest known ionic event during Friend murine erythroleukemic (MEL) cell differentiation along the erythroid pathway is a 45% drop in intracellular sodium concentration ([Na+]i) due to a decrease in Na+ influx (Lannigan, D. A., and Knauf, P. A. (1985) J. Biol. Chem. 260, 7322-7324). We have analyzed the mechanism of the decreased Na+ influx. The Na+ influx in uninduced cells was insensitive to dimethylamiloride, bumetanide, and diisothiocyanostilbene disulfonate. The intracellular pH (pHi) did not change up to 15 h after dimethyl sulfoxide induction, at which time Na+ influx has decreased by approximately 40%; thus, the decrease in Na+ influx is not coupled to a change in pHi. A substantial amount of the decrease in Na+ influx seems to result from a drop in amino acid-dependent Na+ transport. This reduction in amino acid-dependent Na+ influx reflects a decrease in net Na+ influx rather than solely in Na+/Na+ exchange and can account for an appreciable portion of the reduction in [Na+]i seen during differentiation. The drop in amino acid-dependent Na+ influx could not be explained by membrane depolarization but was correlated with a decrease in protein synthesis. Inhibition of protein synthesis in uninduced cells by cycloheximide also caused a decrease in Na+ influx. We conclude that during differentiation the reduction in protein synthesis decreases amino acid-dependent Na+ influx which in turn causes a drop in [Na+]i leading to a reduction in the Na+/K+ pump rate.

Published

1986

20. Electrophoretic separation of different phophosproteins associated with Ca-ATPase and Na, K-ATPase in human red cell ghosts.

Author

Knauf PA, Proverbio F, and Hoffman JF

Subjects

Adult, Autoradiography, Electrophoresis, Polyacrylamide Gel, Humans, Molecular Weight, Phosphorus Radioisotopes, Pronase, Sodium Dodecyl Sulfate, Adenosine Triphosphatases metabolism, Calcium pharmacology, Cell Membrane analysis, Erythrocytes analysis, Phosphoproteins isolation & purification, Potassium pharmacology, Sodium pharmacology

Abstract

Ca has been found to increase the quantity of (32)P incorporated into red cell ghosts from [gamma-(32)P]ATP over the levels obtained by incubation with Mg alone or with Mg + Na, in correlation with the effect of Ca on the associated ATPase activities. When the (32)P-labeled ghosts were solubilized in sodium dodecyl sulfate (SDS) and electrophoresed on acrylamide gels only two bands could be detected either by autoradiography or by counting the sliced gels. The faster moving band (P-2) had the same mobility and the same molecular weight (103,000) as the phosphoprotein found either with Mg alone or with Mg + Na. The slower moving band (P-1) was not found in extensively washed ghosts labeled in the absence of Ca. The molecular weight of P-1 is approximately 150,000. P-1 like P-2 was not affected by pretreatment of intact cells with Pronase before labeling indicating that neither the phosphorylating mechanism nor the phosphoprotein are accessible to externally applied Pronase. The demonstration that a Ca-phosphoprotein is separable from the Na-stimulated phosphoprotein suggests that the Ca-ATPase is distinct from and independent of the Na,K-ATPase. The fact that Ca blocks the dephosphorylation by K of the Na-phosphoprotein indicates that caution is required in interpreting results when the activities of the different phosphoproteins have not been separately determined.

Published

1974

21. Chemical characterization and pronase susceptibility of the Na:K pump-associated phosphoprotein of human red blood cells.

Author

Knauf PA, Proverbio F, and Hoffman JF

Subjects

Adenosine Triphosphatases metabolism, Adult, Binding Sites, Biological Transport, Chemical Phenomena, Chemistry, Electrophoresis, Paper, Electrophoresis, Polyacrylamide Gel, Humans, Hydroxylamines, Magnesium metabolism, Molecular Weight, Ouabain metabolism, Pepsin A, Phosphoproteins analysis, Phosphoproteins biosynthesis, Phosphorus Radioisotopes, Sodium Dodecyl Sulfate, Erythrocytes metabolism, Phosphoproteins isolation & purification, Potassium metabolism, Pronase, Sodium metabolism

Abstract

The phosphoproteins formed by incubation of red cell ghosts with [gamma-(32)P]ATP in the presence of Mg and Na + Mg have been characterized by sodium dodecyl sulfate (SDS)-polyacrylamide gel electrophoresis. The (32)P-labeled phosphoprotein was seen as a single peak confined to the region of the diffuse 90,000 dalton polypeptide band; labeling with Na + Mg considerably increased the quantity of (32)P-phosphoprotein contained in this band relative to labeling with Mg alone. Treatment of intact cells with Pronase known to partially hydrolyze the glycoproteins and the 90,000 daltons polypeptide did not change either the amount or the position of the (32)P-phosphoprotein present in the gels. The molecular weight of the (32)P-phosphoprotein is estimated to be 103,000. Pronase treatment of intact cells also did not significantly alter any of the transport parameters of the membrane such as the K pump flux, ouabain binding, or Na,K-ATPase. In contrast, treatment of ghosts with Pronase not only resulted in drastic alteration of the transport parameters but also inhibited the formation of the phosphoprotein under all conditions. Thus, while the Na:K pump is not intrinsically resistant to Pronase, those elements of the pump which are susceptible are not accessible from the outside of the cell. Further, SDS-polyacrylamide gel electrophoresis after Pronase treatment of intact cells results in a substantial increase in the purification of the phosphoprotein relative to that which was previously possible in ghosts.

Published

1974

22. Synthetic diacylglycerols trigger an increase of intracellular free calcium in promyelocytic HL60 cells.

Author

Restrepo D, Kozody DJ, and Knauf PA

Subjects

Benzofurans, Cell Line, Cell Membrane Permeability, Fura-2, Humans, Inositol metabolism, Inositol 1,4,5-Trisphosphate, Inositol Phosphates metabolism, Kinetics, Leukemia, Promyelocytic, Acute, Potassium metabolism, Sodium metabolism, Spectrometry, Fluorescence, Tetradecanoylphorbol Acetate pharmacology, Calcium metabolism, Diglycerides pharmacology, Glycerides pharmacology

Abstract

Phosphoinositide turnover is known to play an important role in intracellular free calcium homeostasis through the inositol trisphophate-mediated release of calcium from intracellular stores. We find that the other product of phosphoinositide turnover, 1,2-diacylglycerol, elicits an increase in intracellular free calcium in HL60 cells which is due, at least in part, to release of calcium from intracellular stores. This effect is specific for calcium, since intracellular sodium and potassium levels and cellular volume were unaffected. Concomitant with the intracellular calcium increase, we find an increase in cellular inositol trisphosphate levels, suggesting that the effect of diacylglycerol on calcium may be mediated by inositol trisphosphate. Diacylglycerols also stimulate calcium efflux. This stimulation is not simply due to the increase in intracellular calcium. These effects appear not to be mediated through stimulation of a phorbol ester-activatable protein kinase C (Ca2+/phospholipid-dependent enzyme) since phorbol esters do not elicit an increase in cytoplasmic free calcium or an increase in calcium efflux.

Published

1989

23. Transmembrane effects of intracellular chloride on the inhibitory potency of extracellular H2DIDS. Evidence for two conformations of the transport site of the human erythrocyte anion exchange protein.

Author

Furuya W, Tarshis T, Law FY, and Knauf PA

Subjects

4-Acetamido-4'-isothiocyanatostilbene-2,2'-disulfonic Acid analogs & derivatives, Adult, Anion Transport Proteins, Chlorides metabolism, Erythrocytes metabolism, Humans, Hydrogen-Ion Concentration, Intracellular Fluid, Membrane Potentials, Models, Biological, Tissue Distribution, 4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid analogs & derivatives, 4-Acetamido-4'-isothiocyanatostilbene-2,2'-disulfonic Acid pharmacology, Carrier Proteins metabolism, Chlorides pharmacology, Erythrocyte Membrane metabolism, Stilbenes pharmacology

Abstract

The ping-pong model for the red cell anion exchange system postulates that the transport protein band 3 can exist in two different conformations, one in which the transport site faces the cytoplasm (Ei) and another in which it faces the outside medium (Eo). This model predicts that an increase in intracellular chloride should increase the fraction of sites in the outward-facing, unloaded form (Eo). Since external H2DIDS is a competitive inhibitor of chloride exchange that does not cross the membrane, it must bind only to the Eo form. Thus, an increase in Eo should cause an increase in H2DIDS inhibition. When intracellular chloride was increased at constant extracellular chloride, the inhibitory potency of H2DIDS rose, as predicted by the ping-pong model. This increase was not due to the concomitant changes in intracellular pH or membrane potential. When the chloride gradient was reversed, the inhibitory potency of H2DIDS decreased, again in qualitative agreement with the ping-pong model. These data provide support for the ping-pong model and also demonstrate that chloride gradients can be used to change the orientation of the transport protein.

Published

1984

24. Decreased intracellular Na+ concentration is an early event in murine erythroleukemic cell differentiation.

Author

Lannigan DA and Knauf PA

Subjects

Animals, Biological Transport, Active, Cell Differentiation, Cell Line, Friend murine leukemia virus, Kinetics, Leukemia, Erythroblastic, Acute pathology, Mice, Leukemia, Erythroblastic, Acute metabolism, Sodium metabolism

Abstract

A decrease in Na+/K+-pump activity is an early event of Friend murine erythroleukemic (MEL) cell differentiation along the erythroid pathway. This decreased Na+/K+-pump activity has been proposed to be an essential step in differentiation which would cause a rise in intracellular Na+ concentration and then, by means of Na+/Ca2+ exchange, an increase in intracellular Ca2+. An increase in intracellular Ca2+ has been proposed to be essential for induction of differentiation. A critical prediction of this Na+-Ca2+ hypothesis is the rise in intracellular Na+. To test this prediction we have measured intracellular Na+ using a novel triple isotope method involving 3H2O, [14C]sucrose, and 22Na to measure total water, extracellular fluid, and Na+, respectively. 22Na equilibration occurred in less than 10 min. In uninduced cells, intracellular Na+ was 15.2 +/- 2.2 mM (S.D., n = 22); after induction for 14-16 h with dimethyl sulfoxide, intracellular Na+ decreased significantly (p less than 0.0001) to 8.4 +/- 1.4 mM (n = 21). The time course of the decline in intracellular Na+ paralleled that of the decrease in the Na+/K+-pump activity. These results are in direct contradiction to the Na+-Ca2+ hypothesis and suggest that observed changes in Na+/K+-pump activity can be explained solely on the basis of changes in intracellular Na+. The drop in intracellular Na+ is due to a decrease in Na+ influx. We suggest, however, that the decrease in the Na+ influx is not itself an essential event of differentiation, but may be induced by a change in the flux of another ion coupled to Na+.

Published

1985

25. The relationship between anion exchange and net anion flow across the human red blood cell membrane.

Author

Knauf PA, Fuhrmann GF, Rothstein S, and Rothstein A

Subjects

Cell Membrane Permeability drug effects, Electric Conductivity, Humans, Hydrogen-Ion Concentration, Potassium metabolism, Stilbenes pharmacology, Valinomycin pharmacology, Bicarbonates metabolism, Chlorides metabolism, Erythrocyte Membrane metabolism, Erythrocytes metabolism, Hydroxides metabolism, Sulfates metabolism

Abstract

The conductive (net) anion permeability of human red blood cells was determined from net KCl or K2SO4 effluxes into low K+ media at high valinomycin concentrations, conditions under which the salt efflux is limited primarily by the net anion permeability. Disulfonic stilbenes, inhibitors of anion exchange, also inhibited KCl or K2SO4 efflux under these conditions, but were less effective at lower valinomycin concentrations where K+ permeability is the primary limiting factor. Various concentrations of 4,4'-diisothiocyanostilbene-2,2'-disulfonate (DIDS) had similar inhibitory effects on net and exchange sulfate fluxes, both of which were almost completely DIDS sensitive. In the case of Cl-, a high correlation was also found between inhibition of net and exchange fluxes, but in this case about 35% of the net flux was insensitive to DIDS. The net and exchange transport processes differed strikingly in their anion selectivity. Net chloride permeability was only four times as high as net sulfate permeability, whereas chloride exchange is over 10,000 times faster than sulfate exchange. Net OH-permeability, determined by an analogous method, was over four orders of magnitude larger than that of Cl-, but was also sensitive to DIDS. These data and others are discussed in terms of the possibility that a common element may be involved in both net and exchange anion transport.

Published

1977

26. N-(4-azido-2-nitrophenyl)-2-aminoethylsulfonate (NAP-taurine) as a photoaffinity probe for identifying membrane components containing the modifier site of the human red blood cell anion exchange system.

Author

Knauf PA, Breuer W, McCulloch L, and Rothstein A

Subjects

Affinity Labels, Binding Sites drug effects, Chlorides metabolism, Chlorides pharmacology, Erythrocyte Membrane analysis, Erythrocyte Membrane radiation effects, Humans, Light, Nitrobenzenes pharmacology, Sulfates metabolism, Taurine pharmacology, Cell Membrane Permeability, Erythrocyte Membrane metabolism, Erythrocytes metabolism, Membrane Proteins metabolism, Taurine analogs & derivatives

Abstract

Exposure of cells to intense light with the photoactivatable reagent, N-(4-azido-2-nitrophenyl)-2-aminoethylsulfonate (NAP-taurine), present in the external medium results in irreversible inhibition of chloride or sulfate exchange. This irreversible inhibition seems to result from covalent reaction with the same sites to which NAP-taurine binds reversibly in the dark. As shown in the preceding paper, high chloride concentrations decrease the reversible inhibition by NAP-taurine in the dark, in a manner suggesting that NAP-taurine and chloride compete for the modifier site of the anion transport system. In a similar fashion, high chloride concentrations in the medium during exposure to light cause a decrease in both the irreversible binding of NAP-taurine to the membrane and the inhibition of chloride exchange. Most of the chloride-sensitive irreversibly bound NAP-taurine is found in the 95,000 dalton polypeptide known as band 3 and, after pronase treatment of intact cells, in the 65,000 dalton fragment of this protein produced by proteolytic cleavage. After chymotrypsin treatment of ghosts, the NAP-taurine is localized in the 17,000 dalton transmembrane portion of this fragment. Although the possible involvement of minor labeled proteins cannot be rigorously excluded, the modifier site labeled by external NAP-taurine appears, therefore, to be located in the same portion of the 95,000 dalton polypeptide as is the transport site.

Published

1978

27. Asymmetry of the red cell anion exchange system. Different mechanisms of reversible inhibition by N-(4-azido-2-nitrophenyl)-2-aminoethylsulfonate (NAP-taurine) at the inside and outside of the membrane.

Author

Knauf PA, Ship S, Breuer W, McCulloch L, and Rothstein A

Subjects

Binding Sites, Binding, Competitive, Chlorides metabolism, Humans, Membrane Potentials, Nitrobenzenes pharmacology, Nystatin pharmacology, Stilbenes pharmacology, Taurine pharmacology, Water metabolism, Cell Membrane Permeability drug effects, Erythrocyte Membrane drug effects, Erythrocytes drug effects, Taurine analogs & derivatives

Abstract

In the dark, the photoaffinity reagent, N-(4-azido-2-nitrophenyl)-2-aminoethylsulfonate (NAP-taurine), acts as a reversible inhibitor of red cell anion exchange when it is present either within the cell or in the external solution. A detailed analysis of the inhibition kinetics, however, reveals substantial differences in the responses to the probe at the two sides of the membrane. On the inside of the cell, NAP-taurine is a relatively low affinity inhibitor of chloride exchange (Ki = 370 microM). Both the effects of chloride on NAP-taurine inhibition and the affinity of NAP-taurine for the system as a substrate are consistent with the concept that internal NAP-taurine competes with chloride for the substrate site of the anion exchange system. External NAP-taurine, on the other hand, is a far more potent inhibitor of chloride exchange (Ki = 20 microM). It acts at a site of considerably lower affinity for chloride than the substrate site, probably the modifier site, at which halide anions are reported to cause a noncompetitive inhibition of chloride transport. NAP-taurine therefore seems to interact preferentially with either the substrate or modifier site of the transport system, depending on the side of the membrane at which it is present. It is suggested that the modifier site is accessible to NAP-taurine only from the outside whereas the transport site may be accessible from either side.

Published

1978

28. Dog red blood cells exhibit a Ca-stimulated increase in K permeability in the absence of (Na,K)ATPase activity.

Author

Richhardt H, Fuhrmann GF, and Knauf PA

Subjects

Animals, Cell Membrane Permeability drug effects, Osmolar Concentration, Sodium blood, Sodium-Potassium-Exchanging ATPase blood, Calcium pharmacology, Dogs blood, Erythrocyte Membrane physiology, Erythrocytes physiology, Potassium blood

Published

1979

29. Chemical modification of membranes. II. Permeation paths for sulfhydryl agents.

Author

Knauf PA and Rothstein A

Subjects

Cyanides metabolism, Humans, Mercury antagonists & inhibitors, Mercury metabolism, Mercury Isotopes, Organometallic Compounds antagonists & inhibitors, Organometallic Compounds metabolism, Phosphates pharmacology, Sulfates pharmacology, Sulfhydryl Reagents, Sulfonic Acids antagonists & inhibitors, Cell Membrane Permeability drug effects, Sulfhydryl Compounds antagonists & inhibitors, Sulfonic Acids metabolism

Abstract

The amino-reactive reagent, 4-acetamido-4'-isothiocyanostilbene-2,2'-disulfonic acid (SITS),(1) considerably reduces the uptake of the sulfhydryl agent, parachloromercuriphenylsulfonic acid (PCMBS), but does not reduce its effects on cation permeability and on cation transport. These data indicate that PCMBS enters the membrane by at least two channels, one sensitive and the other insensitive to SITS, with only the latter leading to the cation-controlling sulfhydryl groups. Substitution of phosphate or sulfate for chloride results in an inhibition of PCMBS uptake via the SITS-insensitive pathway. These and other data lead to the conclusion that the SITS-sensitive pathway is the predominant one for anion permeation, and the insensitive one for cation permeation. Parachloromercuribenzoate (PCMB), an agent that is more lipid-soluble than PCMBS, penetrates faster but has a smaller effect on cation permeability. Its uptake is less sensitive to SITS. These and other observations suggest that the cation permeation path involves an aqueous channel in the membrane.

Published

1971

30. Chemical modification of membranes. I. Effects of sulfhydryl and amino reactive reagents on anion and cation permeability of the human red blood cell.

Author

Knauf PA and Rothstein A

Subjects

Antimony pharmacology, Binding Sites, Erythrocytes metabolism, Fluorometry, Humans, Mercury pharmacology, Nitrobenzenes pharmacology, Organometallic Compounds pharmacology, Potassium metabolism, Sulfates metabolism, Sulfhydryl Reagents pharmacology, Sulfur Isotopes, Tropanes pharmacology, Cell Membrane Permeability drug effects, Erythrocytes drug effects, Sulfhydryl Compounds antagonists & inhibitors, Sulfonic Acids pharmacology

Abstract

Four different amino-reactive reagents, 4-acetamido-4'-isothiocyano-stilbene-2,2'-disulfonic acid (SITS),(1) 1-fluoro-2,4-dinitrobenzene (FDNB), 2,4,6-trinitrobenzene sulfonic acid (TNBS), and 2-methoxy-5-nitrotropone (MNT) decrease the anion permeability of the human red blood cell, as measured by sulfate fluxes, whereas the sulfhydryl agent, parachloromercuriphenyl sulfonic acid (PCMBS), does not. In contrast, PCMBS increases the cation permeability as measured by K(+) leakage, whereas SITS does not. Of the other agents, FDNB increases the cation permeability to the same extent as PCMBS but MNT and TNBS produce smaller increases. PCMBS does not protect against FDNB as it does against other sulfhydryl agents (X-irradiation) and the FDNB effect on cations is attributed to amino groups. Studies of the binding of SITS indicate that it does not penetrate into the membrane and its failure to influence cation permeability is attributed to its inability to reach an internal population of amino groups. It is concluded that two ion permeability barriers, both involving proteins, are present in the red blood cell. The more superficial barrier contains amino groups and controls anion flow; the more internal barrier contains sulfhydryl and amino groups and controls cation flow. The amino groups contribute to the control of permeability by virtue of their positive charges, but the role of sulfhydryl groups is not clear. Only a small fraction of the membrane protein amino and sulfhydryl is involved in the barriers.

Published

1971