Dynamic Regulation of Cell Volume and Extracellular ATP of Human Erythrocytes

INTRODUCTION: The peptide mastoparan 7 (MST7) triggered in human erythrocytes (rbcs) the release of ATP and swelling. Since swelling is a well-known inducer of ATP release, and extracellular (ATPe), interacting with P (purinergic) receptors, can affect cell volume (Vr), we explored the dynamic regul...

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Autores principales: Leal Denis, M. Florencia, Alvarez, H. Ariel, Lauri, Natalia, Alvarez, Cora L., Chara, Osvaldo, Schwarzbaum, Pablo J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4927150/
https://www.ncbi.nlm.nih.gov/pubmed/27355484
http://dx.doi.org/10.1371/journal.pone.0158305
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author Leal Denis, M. Florencia
Alvarez, H. Ariel
Lauri, Natalia
Alvarez, Cora L.
Chara, Osvaldo
Schwarzbaum, Pablo J.
author_facet Leal Denis, M. Florencia
Alvarez, H. Ariel
Lauri, Natalia
Alvarez, Cora L.
Chara, Osvaldo
Schwarzbaum, Pablo J.
author_sort Leal Denis, M. Florencia
collection PubMed
description INTRODUCTION: The peptide mastoparan 7 (MST7) triggered in human erythrocytes (rbcs) the release of ATP and swelling. Since swelling is a well-known inducer of ATP release, and extracellular (ATPe), interacting with P (purinergic) receptors, can affect cell volume (Vr), we explored the dynamic regulation between Vr and ATPe. METHODS AND TREATMENTS: We made a quantitative assessment of MST7-dependent kinetics of Vr and of [ATPe], both in the absence and presence of blockers of ATP efflux, swelling and P receptors. RESULTS: In rbcs 10 μM MST7 promoted acute, strongly correlated changes in [ATPe] and Vr. Whereas MST7 induced increases of 10% in Vr and 190 nM in [ATPe], blocking swelling in a hyperosmotic medium + MST7 reduced [ATPe] by 40%. Pre-incubation of rbcs with 10 μM of either carbenoxolone or probenecid, two inhibitors of the ATP conduit pannexin 1, reduced [ATPe] by 40–50% and swelling by 40–60%, while in the presence of 80 U/mL apyrase, an ATPe scavenger, cell swelling was prevented. While exposure to 10 μM NF110, a blocker of ATP-P2X receptors mediating sodium influx, reduced [ATPe] by 48%, and swelling by 80%, incubation of cells in sodium free medium reduced swelling by 92%. ANALYSIS AND DISCUSSION: Results were analyzed by means of a mathematical model where ATPe kinetics and Vr kinetics were mutually regulated. Model dependent fit to experimental data showed that, upon MST7 exposure, ATP efflux required a fast 1960-fold increase of ATP permeability, mediated by two kinetically different conduits, both of which were activated by swelling and inactivated by time. Both experimental and theoretical results suggest that, following MST7 exposure, ATP is released via two conduits, one of which is mediated by pannexin 1. The accumulated ATPe activates P2X receptors, followed by sodium influx, resulting in cell swelling, which in turn further activates ATP release. Thus swelling and P2X receptors constitute essential components of a positive feedback loop underlying ATP-induced ATP release of rbcs.
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spelling pubmed-49271502016-07-18 Dynamic Regulation of Cell Volume and Extracellular ATP of Human Erythrocytes Leal Denis, M. Florencia Alvarez, H. Ariel Lauri, Natalia Alvarez, Cora L. Chara, Osvaldo Schwarzbaum, Pablo J. PLoS One Research Article INTRODUCTION: The peptide mastoparan 7 (MST7) triggered in human erythrocytes (rbcs) the release of ATP and swelling. Since swelling is a well-known inducer of ATP release, and extracellular (ATPe), interacting with P (purinergic) receptors, can affect cell volume (Vr), we explored the dynamic regulation between Vr and ATPe. METHODS AND TREATMENTS: We made a quantitative assessment of MST7-dependent kinetics of Vr and of [ATPe], both in the absence and presence of blockers of ATP efflux, swelling and P receptors. RESULTS: In rbcs 10 μM MST7 promoted acute, strongly correlated changes in [ATPe] and Vr. Whereas MST7 induced increases of 10% in Vr and 190 nM in [ATPe], blocking swelling in a hyperosmotic medium + MST7 reduced [ATPe] by 40%. Pre-incubation of rbcs with 10 μM of either carbenoxolone or probenecid, two inhibitors of the ATP conduit pannexin 1, reduced [ATPe] by 40–50% and swelling by 40–60%, while in the presence of 80 U/mL apyrase, an ATPe scavenger, cell swelling was prevented. While exposure to 10 μM NF110, a blocker of ATP-P2X receptors mediating sodium influx, reduced [ATPe] by 48%, and swelling by 80%, incubation of cells in sodium free medium reduced swelling by 92%. ANALYSIS AND DISCUSSION: Results were analyzed by means of a mathematical model where ATPe kinetics and Vr kinetics were mutually regulated. Model dependent fit to experimental data showed that, upon MST7 exposure, ATP efflux required a fast 1960-fold increase of ATP permeability, mediated by two kinetically different conduits, both of which were activated by swelling and inactivated by time. Both experimental and theoretical results suggest that, following MST7 exposure, ATP is released via two conduits, one of which is mediated by pannexin 1. The accumulated ATPe activates P2X receptors, followed by sodium influx, resulting in cell swelling, which in turn further activates ATP release. Thus swelling and P2X receptors constitute essential components of a positive feedback loop underlying ATP-induced ATP release of rbcs. Public Library of Science 2016-06-29 /pmc/articles/PMC4927150/ /pubmed/27355484 http://dx.doi.org/10.1371/journal.pone.0158305 Text en © 2016 Leal Denis et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Leal Denis, M. Florencia
Alvarez, H. Ariel
Lauri, Natalia
Alvarez, Cora L.
Chara, Osvaldo
Schwarzbaum, Pablo J.
Dynamic Regulation of Cell Volume and Extracellular ATP of Human Erythrocytes
title Dynamic Regulation of Cell Volume and Extracellular ATP of Human Erythrocytes
title_full Dynamic Regulation of Cell Volume and Extracellular ATP of Human Erythrocytes
title_fullStr Dynamic Regulation of Cell Volume and Extracellular ATP of Human Erythrocytes
title_full_unstemmed Dynamic Regulation of Cell Volume and Extracellular ATP of Human Erythrocytes
title_short Dynamic Regulation of Cell Volume and Extracellular ATP of Human Erythrocytes
title_sort dynamic regulation of cell volume and extracellular atp of human erythrocytes
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4927150/
https://www.ncbi.nlm.nih.gov/pubmed/27355484
http://dx.doi.org/10.1371/journal.pone.0158305
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