Literature DB >> 24786318

Traction force microscopy in rapidly moving cells reveals separate roles for ROCK and MLCK in the mechanics of retraction.

Timothy R Morin1, Sean A Ghassem-Zadeh1, Juliet Lee2.   

Abstract

Retraction is a major rate-limiting step in cell motility, particularly in slow moving cell types that form large stable adhesions. Myosin II dependent contractile forces are thought to facilitate detachment by physically pulling up the rear edge. However, retraction can occur in the absence of myosin II activity in cell types that form small labile adhesions. To investigate the role of contractile force generation in retraction, we performed traction force microscopy during the movement of fish epithelial keratocytes. By correlating changes in local traction stress at the rear with the area retracted, we identified four distinct modes of retraction. "Recoil" retractions are preceded by a rise in local traction stress, while rear edge is temporarily stuck, followed by a sharp drop in traction stress upon detachment. This retraction type was most common in cells generating high average traction stress. In "pull" type retractions local traction stress and area retracted increase concomitantly. This was the predominant type of retraction in keratocytes and was observed mostly in cells generating low average traction stress. "Continuous" type retractions occur without any detectable change in traction stress, and are seen in cells generating low average traction stress. In contrast, to many other cell types, "release" type retractions occur in keratocytes following a decrease in local traction stress. Our identification of distinct modes of retraction suggests that contractile forces may play different roles in detachment that are related to rear adhesion strength. To determine how the regulation of contractility via MLCK or Rho kinase contributes to the mechanics of detachment, inhibitors were used to block or augment these pathways. Modulation of MLCK activity led to the most rapid change in local traction stress suggesting its importance in regulating attachment strength. Surprisingly, Rho kinase was not required for detachment, but was essential for localizing retraction to the rear. We suggest that in keratocytes MLCK and Rho kinase play distinct, complementary roles in the respective temporal and spatial control of rear detachment that is essential for maintaining rapid motility.
Copyright © 2014 Elsevier Inc. All rights reserved.

Keywords:  Adhesion; Cell motility; Contractility; Mechanics; Retraction; Traction stress

Mesh:

Substances:

Year:  2014        PMID: 24786318     DOI: 10.1016/j.yexcr.2014.04.015

Source DB:  PubMed          Journal:  Exp Cell Res        ISSN: 0014-4827            Impact factor:   3.905


  8 in total

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2.  Comparative mechanisms of cancer cell migration through 3D matrix and physiological microtracks.

Authors:  Shawn P Carey; Aniqua Rahman; Casey M Kraning-Rush; Bethsabe Romero; Sahana Somasegar; Olivia M Torre; Rebecca M Williams; Cynthia A Reinhart-King
Journal:  Am J Physiol Cell Physiol       Date:  2014-12-10       Impact factor: 4.249

3.  Synaptopodin stress fiber and contractomere at the epithelial junction.

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5.  Force transmission during adhesion-independent migration.

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Authors:  Stephanie S Chang; Andrew D Rape; Stephanie A Wong; Wei-Hui Guo; Yu-Li Wang
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7.  Single cell force profiling of human myofibroblasts reveals a biophysical spectrum of cell states.

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Review 8.  Traction force microscopy for understanding cellular mechanotransduction.

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Journal:  BMB Rep       Date:  2020-02       Impact factor: 4.778

  8 in total

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