Silica nanoparticles inhibit the cation channel TRPV4 in airway epithelial cells

Silica nanoparticles inhibit the cation channel TRPV4 in airway epithelial cells

Abstract Background Silica nanoparticles (SiNPs) have numerous beneficial properties and are extensively used in cosmetics and food industries as anti-caking, densifying and hydrophobic agents. However, the increasing exposure levels experienced by the general population and the ability of SiNPs to...

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Main Authors: Alicia Sanchez, Julio L. Alvarez, Kateryna Demydenko, Carole Jung, Yeranddy A. Alpizar, Julio Alvarez-Collazo, Stevan M. Cokic, Miguel A. Valverde, Peter H. Hoet, Karel Talavera
Format: Article
Language:English
Published: BMC 2017-11-01
Series:Particle and Fibre Toxicology
Subjects:
silica nanoparticles
TRPV4
GSK1016790A
epithelial cells
ciliary beat frequency
Online Access:http://link.springer.com/article/10.1186/s12989-017-0224-2
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spelling doaj-1e52881112c64247aefc66db6d2c0ad82020-11-25T00:44:17ZengBMCParticle and Fibre Toxicology1743-89772017-11-0114111410.1186/s12989-017-0224-2Silica nanoparticles inhibit the cation channel TRPV4 in airway epithelial cellsAlicia Sanchez0Julio L. Alvarez1Kateryna Demydenko2Carole Jung3Yeranddy A. Alpizar4Julio Alvarez-Collazo5Stevan M. Cokic6Miguel A. Valverde7Peter H. Hoet8Karel Talavera9Department of Cellular and Molecular Medicine, Laboratory of Ion Channel Research, KU Leuven; VIB Center for Brain & Disease ResearchDepartment of Cellular and Molecular Medicine, Laboratory of Ion Channel Research, KU Leuven; VIB Center for Brain & Disease ResearchDepartment of Cellular and Molecular Medicine, Laboratory of Ion Channel Research, KU Leuven; VIB Center for Brain & Disease ResearchDepartment of Experimental and Health Sciences, Laboratory of Molecular Physiology and Channelopathies, Universitat Pompeu FabraDepartment of Cellular and Molecular Medicine, Laboratory of Ion Channel Research, KU Leuven; VIB Center for Brain & Disease ResearchDepartment of Cellular and Molecular Medicine, Laboratory of Ion Channel Research, KU Leuven; VIB Center for Brain & Disease ResearchKU Leuven BIOMAT, Department of Oral Health Sciences, KU Leuven & Dentistry University Hospitals LeuvenDepartment of Experimental and Health Sciences, Laboratory of Molecular Physiology and Channelopathies, Universitat Pompeu FabraDepartment of Public Health and Primary Care, KU LeuvenDepartment of Cellular and Molecular Medicine, Laboratory of Ion Channel Research, KU Leuven; VIB Center for Brain & Disease ResearchAbstract Background Silica nanoparticles (SiNPs) have numerous beneficial properties and are extensively used in cosmetics and food industries as anti-caking, densifying and hydrophobic agents. However, the increasing exposure levels experienced by the general population and the ability of SiNPs to penetrate cells and tissues have raised concerns about possible toxic effects of this material. Although SiNPs are known to affect the function of the airway epithelium, the molecular targets of these particles remain largely unknown. Given that SiNPs interact with the plasma membrane of epithelial cells we hypothesized that they may affect the function of Transient Receptor Potential Vanilloid 4 (TRPV4), a cation-permeable channel that regulates epithelial barrier function. The main aims of this study were to evaluate the effects of SiNPs on the activation of TRPV4 and to determine whether these alter the positive modulatory action of this channel on the ciliary beat frequency in airway epithelial cells. Results Using fluorometric measurements of intracellular Ca2+ concentration ([Ca2+]i) we found that SiNPs inhibit activation of TRPV4 by the synthetic agonist GSK1016790A in cultured human airway epithelial cells 16HBE and in primary cultured mouse tracheobronchial epithelial cells. Inhibition of TRPV4 by SiNPs was confirmed in intracellular Ca2+ imaging and whole-cell patch-clamp experiments performed in HEK293T cells over-expressing this channel. In addition to these effects, SiNPs were found to induce a significant increase in basal [Ca2+]i, but in a TRPV4-independent manner. SiNPs enhanced the activation of the capsaicin receptor TRPV1, demonstrating that these particles have a specific inhibitory action on TRPV4 activation. Finally, we found that SiNPs abrogate the increase in ciliary beat frequency induced by TRPV4 activation in mouse airway epithelial cells. Conclusions Our results show that SiNPs inhibit TRPV4 activation, and that this effect may impair the positive modulatory action of the stimulation of this channel on the ciliary function in airway epithelial cells. These findings unveil the cation channel TRPV4 as a primary molecular target of SiNPs.http://link.springer.com/article/10.1186/s12989-017-0224-2silica nanoparticlesTRPV4GSK1016790Aepithelial cellsciliary beat frequency
collection DOAJ
language English
format Article
sources DOAJ
author Alicia Sanchez
Julio L. Alvarez
Kateryna Demydenko
Carole Jung
Yeranddy A. Alpizar
Julio Alvarez-Collazo
Stevan M. Cokic
Miguel A. Valverde
Peter H. Hoet
Karel Talavera
spellingShingle Alicia Sanchez
Julio L. Alvarez
Kateryna Demydenko
Carole Jung
Yeranddy A. Alpizar
Julio Alvarez-Collazo
Stevan M. Cokic
Miguel A. Valverde
Peter H. Hoet
Karel Talavera
Silica nanoparticles inhibit the cation channel TRPV4 in airway epithelial cells
Particle and Fibre Toxicology
silica nanoparticles
TRPV4
GSK1016790A
epithelial cells
ciliary beat frequency
author_facet Alicia Sanchez
Julio L. Alvarez
Kateryna Demydenko
Carole Jung
Yeranddy A. Alpizar
Julio Alvarez-Collazo
Stevan M. Cokic
Miguel A. Valverde
Peter H. Hoet
Karel Talavera
author_sort Alicia Sanchez
title Silica nanoparticles inhibit the cation channel TRPV4 in airway epithelial cells
title_short Silica nanoparticles inhibit the cation channel TRPV4 in airway epithelial cells
title_full Silica nanoparticles inhibit the cation channel TRPV4 in airway epithelial cells
title_fullStr Silica nanoparticles inhibit the cation channel TRPV4 in airway epithelial cells
title_full_unstemmed Silica nanoparticles inhibit the cation channel TRPV4 in airway epithelial cells
title_sort silica nanoparticles inhibit the cation channel trpv4 in airway epithelial cells
publisher BMC
series Particle and Fibre Toxicology
issn 1743-8977
publishDate 2017-11-01
description Abstract Background Silica nanoparticles (SiNPs) have numerous beneficial properties and are extensively used in cosmetics and food industries as anti-caking, densifying and hydrophobic agents. However, the increasing exposure levels experienced by the general population and the ability of SiNPs to penetrate cells and tissues have raised concerns about possible toxic effects of this material. Although SiNPs are known to affect the function of the airway epithelium, the molecular targets of these particles remain largely unknown. Given that SiNPs interact with the plasma membrane of epithelial cells we hypothesized that they may affect the function of Transient Receptor Potential Vanilloid 4 (TRPV4), a cation-permeable channel that regulates epithelial barrier function. The main aims of this study were to evaluate the effects of SiNPs on the activation of TRPV4 and to determine whether these alter the positive modulatory action of this channel on the ciliary beat frequency in airway epithelial cells. Results Using fluorometric measurements of intracellular Ca2+ concentration ([Ca2+]i) we found that SiNPs inhibit activation of TRPV4 by the synthetic agonist GSK1016790A in cultured human airway epithelial cells 16HBE and in primary cultured mouse tracheobronchial epithelial cells. Inhibition of TRPV4 by SiNPs was confirmed in intracellular Ca2+ imaging and whole-cell patch-clamp experiments performed in HEK293T cells over-expressing this channel. In addition to these effects, SiNPs were found to induce a significant increase in basal [Ca2+]i, but in a TRPV4-independent manner. SiNPs enhanced the activation of the capsaicin receptor TRPV1, demonstrating that these particles have a specific inhibitory action on TRPV4 activation. Finally, we found that SiNPs abrogate the increase in ciliary beat frequency induced by TRPV4 activation in mouse airway epithelial cells. Conclusions Our results show that SiNPs inhibit TRPV4 activation, and that this effect may impair the positive modulatory action of the stimulation of this channel on the ciliary function in airway epithelial cells. These findings unveil the cation channel TRPV4 as a primary molecular target of SiNPs.
topic silica nanoparticles
TRPV4
GSK1016790A
epithelial cells
ciliary beat frequency
url http://link.springer.com/article/10.1186/s12989-017-0224-2
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