Literature DB >> 20725677

Ultra-rapid activation of TRPV4 ion channels by mechanical forces applied to cell surface beta1 integrins.

Benjamin D Matthews1, Charles K Thodeti, Jessica D Tytell, Akiko Mammoto, Darryl R Overby, Donald E Ingber.   

Abstract

Integrins are ubiquitous transmembrane mechanoreceptors that elicit changes in intracellular biochemistry in response to mechanical force application, but these alterations generally proceed over seconds to minutes. Stress-sensitive ion channels represent another class of mechanoreceptors that are activated much more rapidly (within msec), and recent findings suggest that calcium influx through Transient Receptor Potential Vanilloid-4 (TRPV4) channels expressed in the plasma membrane of bovine capillary endothelial cells is required for mechanical strain-induced changes in focal adhesion assembly, cell orientation and directional migration. However, whether mechanically stretching a cell's extracellular matrix (ECM) adhesions might directly activate cell surface ion channels remains unknown. Here we show that forces applied to beta1 integrins result in ultra-rapid (within 4 msec) activation of calcium influx through TRPV4 channels. The TRPV4 channels were specifically activated by mechanical strain in the cytoskeletal backbone of the focal adhesion, and not by deformation of the lipid bilayer or submembranous cortical cytoskeleton alone. This early-immediate calcium signaling response required the distal region of the beta1 integrin cytoplasmic tail that contains a binding site for the integrin-associated transmembrane CD98 protein, and external force application to CD98 within focal adhesions activated the same ultra-rapid calcium signaling response. Local direct strain-dependent activation of TRPV4 channels mediated by force transfer from integrins and CD98 may therefore enable compartmentalization of calcium signaling within focal adhesions that is critical for mechanical control of many cell behaviors that underlie cell and tissue development.

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Year:  2010        PMID: 20725677      PMCID: PMC3147167          DOI: 10.1039/c0ib00034e

Source DB:  PubMed          Journal:  Integr Biol (Camb)        ISSN: 1757-9694            Impact factor:   2.192


  45 in total

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Review 4.  Cell adhesion receptors in mechanotransduction.

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6.  The PKD1 gene product, "polycystin-1," is a tyrosine-phosphorylated protein that colocalizes with alpha2beta1-integrin in focal clusters in adherent renal epithelia.

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7.  TRPV4 channels mediate cyclic strain-induced endothelial cell reorientation through integrin-to-integrin signaling.

Authors:  Charles K Thodeti; Benjamin Matthews; Arvind Ravi; Akiko Mammoto; Kaustabh Ghosh; Abigail L Bracha; Donald E Ingber
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Review 8.  Integrin-associated proteins as potential therapeutic targets.

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9.  Integrin-linked kinase is localized to cell-matrix focal adhesions but not cell-cell adhesion sites and the focal adhesion localization of integrin-linked kinase is regulated by the PINCH-binding ANK repeats.

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Review 6.  Stretch-induced actomyosin contraction in epithelial tubes: Mechanotransduction pathways for tubular homeostasis.

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7.  Modeling the two-way feedback between contractility and matrix realignment reveals a nonlinear mode of cancer cell invasion.

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8.  Prevention of ventilator-induced lung edema by inhalation of nanoparticles releasing ruthenium red.

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10.  Update on vascular endothelial Ca(2+) signalling: A tale of ion channels, pumps and transporters.

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