Stable potassium isotopes ((41)K/(39)K) track transcellular and paracellular potassium transport in biological systems

As the most abundant cation in archaeal, bacterial, and eukaryotic cells, potassium (K(+)) is an essential element for life. While much is known about the machinery of transcellular and paracellular K transport–channels, pumps, co-transporters, and tight-junction proteins—many quantitative aspects o...

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Autores principales: Higgins, John A., Ramos, Danielle Santiago, Gili, Stefania, Spetea, Cornelia, Kanoski, Scott, Ha, Darren, McDonough, Alicia A., Youn, Jang H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Physiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9644202/
https://www.ncbi.nlm.nih.gov/pubmed/36388124
http://dx.doi.org/10.3389/fphys.2022.1016242
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author Higgins, John A.
Ramos, Danielle Santiago
Gili, Stefania
Spetea, Cornelia
Kanoski, Scott
Ha, Darren
McDonough, Alicia A.
Youn, Jang H.
author_facet Higgins, John A.
Ramos, Danielle Santiago
Gili, Stefania
Spetea, Cornelia
Kanoski, Scott
Ha, Darren
McDonough, Alicia A.
Youn, Jang H.
author_sort Higgins, John A.
collection PubMed
description As the most abundant cation in archaeal, bacterial, and eukaryotic cells, potassium (K(+)) is an essential element for life. While much is known about the machinery of transcellular and paracellular K transport–channels, pumps, co-transporters, and tight-junction proteins—many quantitative aspects of K homeostasis in biological systems remain poorly constrained. Here we present measurements of the stable isotope ratios of potassium ((41)K/(39)K) in three biological systems (algae, fish, and mammals). When considered in the context of our current understanding of plausible mechanisms of K isotope fractionation and K(+) transport in these biological systems, our results provide evidence that the fractionation of K isotopes depends on transport pathway and transmembrane transport machinery. Specifically, we find that passive transport of K(+) down its electrochemical potential through channels and pores in tight-junctions at favors (39)K, a result which we attribute to a kinetic isotope effect associated with dehydration and/or size selectivity at the channel/pore entrance. In contrast, we find that transport of K(+) against its electrochemical gradient via pumps and co-transporters is associated with less/no isotopic fractionation, a result that we attribute to small equilibrium isotope effects that are expressed in pumps/co-transporters due to their slower turnover rate and the relatively long residence time of K(+) in the ion pocket. These results indicate that stable K isotopes may be able to provide quantitative constraints on transporter-specific K(+) fluxes (e.g., the fraction of K efflux from a tissue by channels vs. co-transporters) and how these fluxes change in different physiological states. In addition, precise determination of K isotope effects associated with K(+) transport via channels, pumps, and co-transporters may provide unique constraints on the mechanisms of K transport that could be tested with steered molecular dynamic simulations.
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spelling pubmed-96442022022-11-15 Stable potassium isotopes ((41)K/(39)K) track transcellular and paracellular potassium transport in biological systems Higgins, John A. Ramos, Danielle Santiago Gili, Stefania Spetea, Cornelia Kanoski, Scott Ha, Darren McDonough, Alicia A. Youn, Jang H. Front Physiol Physiology As the most abundant cation in archaeal, bacterial, and eukaryotic cells, potassium (K(+)) is an essential element for life. While much is known about the machinery of transcellular and paracellular K transport–channels, pumps, co-transporters, and tight-junction proteins—many quantitative aspects of K homeostasis in biological systems remain poorly constrained. Here we present measurements of the stable isotope ratios of potassium ((41)K/(39)K) in three biological systems (algae, fish, and mammals). When considered in the context of our current understanding of plausible mechanisms of K isotope fractionation and K(+) transport in these biological systems, our results provide evidence that the fractionation of K isotopes depends on transport pathway and transmembrane transport machinery. Specifically, we find that passive transport of K(+) down its electrochemical potential through channels and pores in tight-junctions at favors (39)K, a result which we attribute to a kinetic isotope effect associated with dehydration and/or size selectivity at the channel/pore entrance. In contrast, we find that transport of K(+) against its electrochemical gradient via pumps and co-transporters is associated with less/no isotopic fractionation, a result that we attribute to small equilibrium isotope effects that are expressed in pumps/co-transporters due to their slower turnover rate and the relatively long residence time of K(+) in the ion pocket. These results indicate that stable K isotopes may be able to provide quantitative constraints on transporter-specific K(+) fluxes (e.g., the fraction of K efflux from a tissue by channels vs. co-transporters) and how these fluxes change in different physiological states. In addition, precise determination of K isotope effects associated with K(+) transport via channels, pumps, and co-transporters may provide unique constraints on the mechanisms of K transport that could be tested with steered molecular dynamic simulations. Frontiers Media S.A. 2022-10-26 /pmc/articles/PMC9644202/ /pubmed/36388124 http://dx.doi.org/10.3389/fphys.2022.1016242 Text en Copyright © 2022 Higgins, Ramos, Gili, Spetea, Kanoski, Ha, McDonough and Youn. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Physiology
Higgins, John A.
Ramos, Danielle Santiago
Gili, Stefania
Spetea, Cornelia
Kanoski, Scott
Ha, Darren
McDonough, Alicia A.
Youn, Jang H.
Stable potassium isotopes ((41)K/(39)K) track transcellular and paracellular potassium transport in biological systems
title Stable potassium isotopes ((41)K/(39)K) track transcellular and paracellular potassium transport in biological systems
title_full Stable potassium isotopes ((41)K/(39)K) track transcellular and paracellular potassium transport in biological systems
title_fullStr Stable potassium isotopes ((41)K/(39)K) track transcellular and paracellular potassium transport in biological systems
title_full_unstemmed Stable potassium isotopes ((41)K/(39)K) track transcellular and paracellular potassium transport in biological systems
title_short Stable potassium isotopes ((41)K/(39)K) track transcellular and paracellular potassium transport in biological systems
title_sort stable potassium isotopes ((41)k/(39)k) track transcellular and paracellular potassium transport in biological systems
topic Physiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9644202/
https://www.ncbi.nlm.nih.gov/pubmed/36388124
http://dx.doi.org/10.3389/fphys.2022.1016242
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