Your search keyword '"Bazzone, Andre"' showing total 5 results

1. Unraveling the kinetics and pharmacology of human PepT1 using solid supported membrane-based electrophysiology.

Author

Körner A, Bazzone A, Wichert M, Barthmes M, Dondapati SK, Fertig N, and Kubick S

Subjects

Humans, Peptide Transporter 1, Electrophysiology, Peptides, Kinetics, Symporters metabolism

Abstract

The human Peptide Transporter 1 (hPepT1) is known for its broad substrate specificity and its ability to transport (pro-)drugs. Here, we present an in-depth comprehensive study of hPepT1 and its interactions with various substrates via solid supported membrane-based electrophysiology (SSME). Using hPepT1-containing vesicles, we could not identify any peptide induced pre-steady-state currents, indicating that the recorded peak currents reflect steady-state transport. Electrogenic co-transport of H + /glycylglycine (GlyGly) was observed across a pH range of 5.0 to 9.0. The pH dependence is described by a bell-shaped activity curve and two pK values. K M and relative V max values of various canonical and non-canonical peptide substrates were contextualized with current mechanistic understandings of hPepT1. Finally, specific inhibition was observed for various inhibitors in a high throughput format, and IC50 values are reported. Taken together, these findings contribute to promoting the design and analysis of pharmacologically relevant substances., Competing Interests: Declaration of Competing Interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Authors AB, MB and NF are employed by Nanion Technologies GmbH, the developer of the SURFE(2)R instruments., (Copyright © 2023 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2024

2. Investigation of sugar binding kinetics of the E. coli sugar/H + symporter XylE using solid-supported membrane-based electrophysiology.

Author

Bazzone A, Tesmer L, Kurt D, Kaback HR, Fendler K, and Madej MG

Subjects

Carbohydrate Metabolism, Electrophysiology, Glucose metabolism, Kinetics, Membrane Transport Proteins genetics, Membrane Transport Proteins metabolism, Sugars metabolism, Escherichia coli genetics, Escherichia coli metabolism, Escherichia coli Proteins metabolism, Monosaccharide Transport Proteins metabolism, Symporters metabolism

Abstract

Bacterial transporters are difficult to study using conventional electrophysiology because of their low transport rates and the small size of bacterial cells. Here, we applied solid-supported membrane-based electrophysiology to derive kinetic parameters of sugar translocation by the Escherichia coli xylose permease (XylE), including functionally relevant mutants. Many aspects of the fucose permease (FucP) and lactose permease (LacY) have also been investigated, which allow for more comprehensive conclusions regarding the mechanism of sugar translocation by transporters of the major facilitator superfamily. In all three of these symporters, we observed sugar binding and transport in real time to determine K M , V max , K D , and k obs values for different sugar substrates. K D and k obs values were attainable because of a conserved sugar-induced electrogenic conformational transition within these transporters. We also analyzed interactions between the residues in the available X-ray sugar/H + symporter structures obtained with different bound sugars. We found that different sugars induce different conformational states, possibly correlating with different charge displacements in the electrophysiological assay upon sugar binding. Finally, we found that mutations in XylE altered the kinetics of glucose binding and transport, as Q175 and L297 are necessary for uncoupling H + and d-glucose translocation. Based on the rates for the electrogenic conformational transition upon sugar binding (>300 s -1 ) and for sugar translocation (2 s -1  - 30 s -1 for different substrates), we propose a multiple-step mechanism and postulate an energy profile for sugar translocation. We also suggest a mechanism by which d-glucose can act as an inhibitor for XylE., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

3. pH Regulation of Electrogenic Sugar/H+ Symport in MFS Sugar Permeases.

Author

Bazzone A, Madej MG, Kaback HR, and Fendler K

Subjects

Biological Transport, Active physiology, Escherichia coli genetics, Escherichia coli Proteins genetics, Hydrogen-Ion Concentration, Monosaccharide Transport Proteins genetics, Symporters genetics, Escherichia coli metabolism, Escherichia coli Proteins metabolism, Monosaccharide Transport Proteins metabolism, Proton-Motive Force physiology, Symporters metabolism

Abstract

Bacterial sugar symporters in the Major Facilitator Superfamily (MFS) use the H+ (and in a few cases Na+) electrochemical gradients to achieve active transport of sugar into the cell. Because a number of structures of MFS sugar symporters have been solved recently, molecular insight into the transport mechanism is possible from detailed functional analysis. We present here a comparative electrophysiological study of the lactose permease (LacY), the fucose permease (FucP) and the xylose permease (XylE), which reveals common mechanistic principles and differences. In all three symporters energetically downhill electrogenic sugar/H+ symport is observed. Comparison of the pH dependence of symport at symmetrical pH exhibits broad bell-shaped pH profiles extending over 3 to 6 pH units and a decrease at extremely alkaline pH ≥ 9.4 and at acidic to neutral pH = 4.6-7.5. The pH dependence can be described by an acidic to neutral apparent pK (pKapp) and an alkaline pKapp. Experimental evidence suggests that the alkaline pKapp is due to H+ depletion at the protonation site, while the acidic pKapp is due to inhibition of deprotonation. Since previous studies suggest that a single carboxyl group in LacY (Glu325) may be the only side chain directly involved in H+ translocation and a carboxyl side chain with similar properties has been identified in FucP (Asp46) and XylE (Asp27), the present results imply that the pK of this residue is switched during H+/sugar symport in all three symporters.

Published

2016

4. Electrophysiological characterization of uncoupled mutants of LacY.

Author

Gaiko O, Bazzone A, Fendler K, and Kaback HR

Subjects

Electrophysiological Phenomena, Escherichia coli Proteins genetics, Escherichia coli Proteins physiology, Lactose metabolism, Liposomes metabolism, Models, Molecular, Mutagenesis, Site-Directed, Proteolipids metabolism, Membrane Transport Proteins genetics, Membrane Transport Proteins physiology, Symporters metabolism

Abstract

In this study of the lactose permease of Escherichia coli (LacY), five functionally irreplaceable residues involved specifically in H(+) translocation (Arg302 and Glu325) or in the coupling between protonation and sugar binding (Tyr236, Glu269, and His322) were mutated individually or together with mutant Glu325 → Ala. The wild type and each mutant were purified and reconstituted into proteoliposomes, which were then examined using solid-supported-membrane-based electrophysiology. Mutants Glu325 → Ala or Arg302 → Ala, in which H(+) symport is abolished, exhibit a weakly electrogenic rapid reaction triggered by sugar binding. The reaction is essentially absent in mutant Tyr236 → Phe, Glu269 → Ala, and His322 → Ala, and each of these mutations blocks the electrogenic reaction observed in the Glu325 → Ala mutant. The findings are consistent with the interpretation that the electrogenic reaction induced by sugar binding is due to rearrangement of charged residues in LacY and that this reaction is blocked by mutation of each member of the Tyr236/Glu269/His322 triad. In addition, further support is provided for the conclusion that deprotonation is rate limiting for downhill lactose/H(+) symport.

Published

2013

5. pH Regulation of Electrogenic Sugar/H+ Symport in MFS Sugar Permeases

Author

Bazzone, Andre, Madej, M. Gregor, Kaback, H. Ronald, Fendler, Klaus, and Gerós, Hernâni

Subjects

Symporters, Monosaccharide Transport Proteins, Active, General Science & Technology, ddc:570, Escherichia coli Proteins, Escherichia coli, Proton-Motive Force, Biological Transport, Hydrogen-Ion Concentration

Abstract

Bacterial sugar symporters in the Major Facilitator Superfamily (MFS) use the H+ (and in a few cases Na+) electrochemical gradients to achieve active transport of sugar into the cell. Because a number of structures of MFS sugar symporters have been solved recently, molecular insight into the transport mechanism is possible from detailed functional analysis. We present here a comparative electrophysiological study of the lactose permease (LacY), the fucose permease (FucP) and the xylose permease (XylE), which reveals common mechanistic principles and differences. In all three symporters energetically downhill electrogenic sugar/H+ symport is observed. Comparison of the pH dependence of symport at symmetrical pH exhibits broad bell-shaped pH profiles extending over 3 to 6 pH units and a decrease at extremely alkaline pH ≥ 9.4 and at acidic to neutral pH = 4.6–7.5. The pH dependence can be described by an acidic to neutral apparent pK (pKapp) and an alkaline pKapp. Experimental evidence suggests that the alkaline pKapp is due to H+ depletion at the protonation site, while the acidic pKapp is due to inhibition of deprotonation. Since previous studies suggest that a single carboxyl group in LacY (Glu325) may be the only side chain directly involved in H+ translocation and a carboxyl side chain with similar properties has been identified in FucP (Asp46) and XylE (Asp27), the present results imply that the pK of this residue is switched during H+/sugar symport in all three symporters.

Published

2016