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  4. The N-terminal Ac-EEED sequence plays a role in alpha-smooth-muscle actin incorporation into stress fibers
 
research article

The N-terminal Ac-EEED sequence plays a role in alpha-smooth-muscle actin incorporation into stress fibers

Clément, Sophie
•
Hinz, Boris
•
Dugina, Vera
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2005
Journal of cell science

We have previously shown that the N-terminal sequence AcEEED of alpha-smooth-muscle actin causes the loss of alpha-smooth-muscle actin from stress fibers and a decrease in cell contractility when introduced in myofibroblasts as a cell-penetrating fusion peptide. Here, we have investigated the function of this sequence on stress fiber organization in living cells, using enhanced green fluorescent protein (EGFP)-tagged alpha-smooth-muscle actin. The fusion peptide provokes the gradual disappearance of EGFP fluorescence of alpha-smooth-muscle actin from stress fibers and the formation of hitherto unknown rod-like structures. In addition to alpha-smooth-muscle actin, these structures contain cytoplasmic actins, gelsolin and cofilin but not other major actin-binding proteins. These rod-like structures are also visible in wild-type fibroblasts during normal cell spreading, suggesting that they represent a physiological step in the organization of alpha-smooth-muscle actin in stress fibers. Fluorescence-recovery-after-photobleaching experiments suggest that the fusion peptide reduces the dynamics of alpha-smooth-muscle actin and its incorporation in stress fibers. Here, we propose a new mechanism of how alpha-smooth-muscle actin is incorporated in stress fibers involving the sequence Ac-EEED.

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Type
research article
DOI
10.1242/jcs.01732
Web of Science ID

WOS:000228631000010

Author(s)
Clément, Sophie
Hinz, Boris
Dugina, Vera
Gabbiani, Giulio
Chaponnier, Christine
Date Issued

2005

Publisher

Company of Biologists

Published in
Journal of cell science
Volume

118

Issue

7

Start page

1395

End page

404

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LCB  
Available on Infoscience
March 25, 2010
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/48792
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