TRPC1‐mediated Ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with PP2Ac after wounding

TRPC1‐mediated Ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with PP2Ac after wounding

Abstract Gut epithelial restitution after superficial wounding is an important repair modality regulated by numerous factors including Ca2+ signaling and cellular polyamines. Transient receptor potential canonical‐1 (TRPC1) functions as a store‐operated Ca2+ channel in intestinal epithelial cells (I...

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Main Authors: Navneeta Rathor, Hee Kyoung Chung, Jia‐Le Song, Shelley R. Wang, Jian‐Ying Wang, Jaladanki N. Rao
Format: Article
Language:English
Published: Wiley 2021-05-01
Series:Physiological Reports
Subjects:
cell migration
epithelial restitution
IEC‐6 cells
mucosal injury
ornithine decarboxylase
polyamines
Online Access:https://doi.org/10.14814/phy2.14864
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spelling doaj-86abe98f503b450e907781a696f662862021-05-15T16:41:05ZengWileyPhysiological Reports2051-817X2021-05-0199n/an/a10.14814/phy2.14864TRPC1‐mediated Ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with PP2Ac after woundingNavneeta Rathor0Hee Kyoung Chung1Jia‐Le Song2Shelley R. Wang3Jian‐Ying Wang4Jaladanki N. Rao5Cell Biology Group, Department of Surgery University of Maryland School of Medicine Baltimore MD USACell Biology Group, Department of Surgery University of Maryland School of Medicine Baltimore MD USACell Biology Group, Department of Surgery University of Maryland School of Medicine Baltimore MD USABaltimore Veterans Affairs Medical Center Baltimore MD USACell Biology Group, Department of Surgery University of Maryland School of Medicine Baltimore MD USACell Biology Group, Department of Surgery University of Maryland School of Medicine Baltimore MD USAAbstract Gut epithelial restitution after superficial wounding is an important repair modality regulated by numerous factors including Ca2+ signaling and cellular polyamines. Transient receptor potential canonical‐1 (TRPC1) functions as a store‐operated Ca2+ channel in intestinal epithelial cells (IECs) and its activation increases epithelial restitution by inducing Ca2+ influx after acute injury. α4 is a multiple functional protein and implicated in many aspects of cell functions by modulating protein phosphatase 2A (PP2A) stability and activity. Here we show that the clonal populations of IECs stably expressing TRPC1 (IEC‐TRPC1) exhibited increased levels of α4 and PP2A catalytic subunit (PP2Ac) and that TRPC1 promoted intestinal epithelial restitution by increasing α4/PP2Ac association. The levels of α4 and PP2Ac proteins increased significantly in stable IEC‐TRPC1 cells and this induction in α4/PP2Ac complexes was accompanied by an increase in IEC migration after wounding. α4 silencing by transfection with siRNA targeting α4 (siα4) or PP2Ac silencing destabilized α4/PP2Ac complexes in stable IEC‐TRPC1 cells and repressed cell migration over the wounded area. Increasing the levels of cellular polyamines by stable transfection with the Odc gene stimulated α4 and PP2Ac expression and enhanced their association, thus also promoting epithelial restitution after wounding. In contrast, depletion of cellular polyamines by treatment with α‐difluoromethylornithine reduced α4/PP2Ac complexes and repressed cell migration. Ectopic overexpression of α4 partially rescued rapid epithelial repair in polyamine‐deficient cells. These results indicate that activation of TRPC1‐mediated Ca2+ signaling enhances cell migration primarily by increasing α4/PP2Ac associations after wounding and this pathway is tightly regulated by cellular polyamines.https://doi.org/10.14814/phy2.14864cell migrationepithelial restitutionIEC‐6 cellsmucosal injuryornithine decarboxylasepolyamines
collection DOAJ
language English
format Article
sources DOAJ
author Navneeta Rathor
Hee Kyoung Chung
Jia‐Le Song
Shelley R. Wang
Jian‐Ying Wang
Jaladanki N. Rao
spellingShingle Navneeta Rathor
Hee Kyoung Chung
Jia‐Le Song
Shelley R. Wang
Jian‐Ying Wang
Jaladanki N. Rao
TRPC1‐mediated Ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with PP2Ac after wounding
Physiological Reports
cell migration
epithelial restitution
IEC‐6 cells
mucosal injury
ornithine decarboxylase
polyamines
author_facet Navneeta Rathor
Hee Kyoung Chung
Jia‐Le Song
Shelley R. Wang
Jian‐Ying Wang
Jaladanki N. Rao
author_sort Navneeta Rathor
title TRPC1‐mediated Ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with PP2Ac after wounding
title_short TRPC1‐mediated Ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with PP2Ac after wounding
title_full TRPC1‐mediated Ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with PP2Ac after wounding
title_fullStr TRPC1‐mediated Ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with PP2Ac after wounding
title_full_unstemmed TRPC1‐mediated Ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with PP2Ac after wounding
title_sort trpc1‐mediated ca2+ signaling enhances intestinal epithelial restitution by increasing α4 association with pp2ac after wounding
publisher Wiley
series Physiological Reports
issn 2051-817X
publishDate 2021-05-01
description Abstract Gut epithelial restitution after superficial wounding is an important repair modality regulated by numerous factors including Ca2+ signaling and cellular polyamines. Transient receptor potential canonical‐1 (TRPC1) functions as a store‐operated Ca2+ channel in intestinal epithelial cells (IECs) and its activation increases epithelial restitution by inducing Ca2+ influx after acute injury. α4 is a multiple functional protein and implicated in many aspects of cell functions by modulating protein phosphatase 2A (PP2A) stability and activity. Here we show that the clonal populations of IECs stably expressing TRPC1 (IEC‐TRPC1) exhibited increased levels of α4 and PP2A catalytic subunit (PP2Ac) and that TRPC1 promoted intestinal epithelial restitution by increasing α4/PP2Ac association. The levels of α4 and PP2Ac proteins increased significantly in stable IEC‐TRPC1 cells and this induction in α4/PP2Ac complexes was accompanied by an increase in IEC migration after wounding. α4 silencing by transfection with siRNA targeting α4 (siα4) or PP2Ac silencing destabilized α4/PP2Ac complexes in stable IEC‐TRPC1 cells and repressed cell migration over the wounded area. Increasing the levels of cellular polyamines by stable transfection with the Odc gene stimulated α4 and PP2Ac expression and enhanced their association, thus also promoting epithelial restitution after wounding. In contrast, depletion of cellular polyamines by treatment with α‐difluoromethylornithine reduced α4/PP2Ac complexes and repressed cell migration. Ectopic overexpression of α4 partially rescued rapid epithelial repair in polyamine‐deficient cells. These results indicate that activation of TRPC1‐mediated Ca2+ signaling enhances cell migration primarily by increasing α4/PP2Ac associations after wounding and this pathway is tightly regulated by cellular polyamines.
topic cell migration
epithelial restitution
IEC‐6 cells
mucosal injury
ornithine decarboxylase
polyamines
url https://doi.org/10.14814/phy2.14864
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AT heekyoungchung trpc1mediatedca2signalingenhancesintestinalepithelialrestitutionbyincreasinga4associationwithpp2acafterwounding
AT jialesong trpc1mediatedca2signalingenhancesintestinalepithelialrestitutionbyincreasinga4associationwithpp2acafterwounding
AT shelleyrwang trpc1mediatedca2signalingenhancesintestinalepithelialrestitutionbyincreasinga4associationwithpp2acafterwounding
AT jianyingwang trpc1mediatedca2signalingenhancesintestinalepithelialrestitutionbyincreasinga4associationwithpp2acafterwounding
AT jaladankinrao trpc1mediatedca2signalingenhancesintestinalepithelialrestitutionbyincreasinga4associationwithpp2acafterwounding
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