Protective role of FKBP51 in calcium entry-induced endothelial barrier disruption

Protective role of FKBP51 in calcium entry-induced endothelial barrier disruption

Pulmonary artery endothelial cells (PAECs) express a cation current, I SOC (store-operated calcium entry current), which when activated permits calcium entry leading to inter-endothelial cell gap formation. The large molecular weight immunophilin FKBP51 inhibits I SOC but not other calcium entry pat...

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Main Authors: Caleb L. Hamilton, Pierre I. Kadeba, Audrey A. Vasauskas, Viktoriya Solodushko, Anna K. McClinton, Mikhail Alexeyev, Jonathan G. Scammell, Donna L. Cioffi
Format: Article
Language:English
Published: SAGE Publishing 2018-01-01
Series:Pulmonary Circulation
Online Access:https://doi.org/10.1177/2045893217749987
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spelling doaj-ffeaf94c49fb46f39d598842735f275e2020-11-25T03:35:15ZengSAGE PublishingPulmonary Circulation2045-89402018-01-01810.1177/2045893217749987Protective role of FKBP51 in calcium entry-induced endothelial barrier disruptionCaleb L. Hamilton0Pierre I. Kadeba1Audrey A. Vasauskas2Viktoriya Solodushko3Anna K. McClinton4Mikhail Alexeyev5Jonathan G. Scammell6Donna L. Cioffi7Center for Lung Biology, University of South Alabama, Mobile, AL, USACenter for Lung Biology, University of South Alabama, Mobile, AL, USA, Alabama College of Osteopathic Medicine, Dothan, AL, USA, University of South Alabama, Mobile, AL, USADepartment of Pharmacology, University of South Alabama, Mobile, AL, USADepartment of Physiology and Cell Biology, University of South Alabama, Mobile, AL, USADepartment of Comparative Medicine, , Mobile, AL, USACenter for Lung Biology, University of South Alabama, Mobile, AL, USAPulmonary artery endothelial cells (PAECs) express a cation current, I SOC (store-operated calcium entry current), which when activated permits calcium entry leading to inter-endothelial cell gap formation. The large molecular weight immunophilin FKBP51 inhibits I SOC but not other calcium entry pathways in PAECs. However, it is unknown whether FKBP51-mediated inhibition of I SOC is sufficient to protect the endothelial barrier from calcium entry-induced disruption. The major objective of this study was to determine whether FKBP51-mediated inhibition of I SOC leads to decreased calcium entry-induced inter-endothelial gap formation and thus preservation of the endothelial barrier. Here, we measured the effects of thapsigargin-induced I SOC on the endothelial barrier in control and FKBP51 overexpressing PAECs. FKBP51 overexpression decreased actin stress fiber and inter-endothelial cell gap formation in addition to attenuating the decrease in resistance observed with control cells using electric cell-substrate impedance sensing. Finally, the thapsigargin-induced increase in dextran flux was abolished in FKBP51 overexpressing PAECs. We then measured endothelial permeability in perfused lungs of FKBP51 knockout (FKBP51 –/– ) mice and observed increased calcium entry-induced permeability compared to wild-type mice. To begin to dissect the mechanism underlying the FKBP51-mediated inhibition of I SOC , a second goal of this study was to determine the role of the microtubule network. We observed that FKBP51 overexpressing PAECs exhibited increased microtubule polymerization that is critical for inhibition of I SOC by FKBP51. Overall, we have identified FKBP51 as a novel regulator of endothelial barrier integrity, and these findings are significant as they reveal a protective mechanism for endothelium against calcium entry-induced disruption.https://doi.org/10.1177/2045893217749987
collection DOAJ
language English
format Article
sources DOAJ
author Caleb L. Hamilton
Pierre I. Kadeba
Audrey A. Vasauskas
Viktoriya Solodushko
Anna K. McClinton
Mikhail Alexeyev
Jonathan G. Scammell
Donna L. Cioffi
spellingShingle Caleb L. Hamilton
Pierre I. Kadeba
Audrey A. Vasauskas
Viktoriya Solodushko
Anna K. McClinton
Mikhail Alexeyev
Jonathan G. Scammell
Donna L. Cioffi
Protective role of FKBP51 in calcium entry-induced endothelial barrier disruption
Pulmonary Circulation
author_facet Caleb L. Hamilton
Pierre I. Kadeba
Audrey A. Vasauskas
Viktoriya Solodushko
Anna K. McClinton
Mikhail Alexeyev
Jonathan G. Scammell
Donna L. Cioffi
author_sort Caleb L. Hamilton
title Protective role of FKBP51 in calcium entry-induced endothelial barrier disruption
title_short Protective role of FKBP51 in calcium entry-induced endothelial barrier disruption
title_full Protective role of FKBP51 in calcium entry-induced endothelial barrier disruption
title_fullStr Protective role of FKBP51 in calcium entry-induced endothelial barrier disruption
title_full_unstemmed Protective role of FKBP51 in calcium entry-induced endothelial barrier disruption
title_sort protective role of fkbp51 in calcium entry-induced endothelial barrier disruption
publisher SAGE Publishing
series Pulmonary Circulation
issn 2045-8940
publishDate 2018-01-01
description Pulmonary artery endothelial cells (PAECs) express a cation current, I SOC (store-operated calcium entry current), which when activated permits calcium entry leading to inter-endothelial cell gap formation. The large molecular weight immunophilin FKBP51 inhibits I SOC but not other calcium entry pathways in PAECs. However, it is unknown whether FKBP51-mediated inhibition of I SOC is sufficient to protect the endothelial barrier from calcium entry-induced disruption. The major objective of this study was to determine whether FKBP51-mediated inhibition of I SOC leads to decreased calcium entry-induced inter-endothelial gap formation and thus preservation of the endothelial barrier. Here, we measured the effects of thapsigargin-induced I SOC on the endothelial barrier in control and FKBP51 overexpressing PAECs. FKBP51 overexpression decreased actin stress fiber and inter-endothelial cell gap formation in addition to attenuating the decrease in resistance observed with control cells using electric cell-substrate impedance sensing. Finally, the thapsigargin-induced increase in dextran flux was abolished in FKBP51 overexpressing PAECs. We then measured endothelial permeability in perfused lungs of FKBP51 knockout (FKBP51 –/– ) mice and observed increased calcium entry-induced permeability compared to wild-type mice. To begin to dissect the mechanism underlying the FKBP51-mediated inhibition of I SOC , a second goal of this study was to determine the role of the microtubule network. We observed that FKBP51 overexpressing PAECs exhibited increased microtubule polymerization that is critical for inhibition of I SOC by FKBP51. Overall, we have identified FKBP51 as a novel regulator of endothelial barrier integrity, and these findings are significant as they reveal a protective mechanism for endothelium against calcium entry-induced disruption.
url https://doi.org/10.1177/2045893217749987
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