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Biophys. J. BioFAST: First Published April 22, 2005. doi:10.1529/biophysj.104.054320
© 2005 by the Biophysical Society.


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CELL BIOPHYSICS

The Dynamics and Mechanics of Endothelial Cell Spreading

Daniel Hammer 1*, Micah Dembo 2 and Cynthia Reinhart-King 1

1 University of Pennsylvania
2 Boston University

* To whom correspondence should be addressed. E-mail: hammer{at}seas.upenn.edu.

Submitted on October 11, 2004
Revised on December 9, 2004
Accepted on 24 March 2005


   Abstract
Cell adhesion to extracellular matrix is mediated by receptor-ligand interactions. When a cell first contacts a surface, it spreads, exerting traction forces against the surface and forming new bonds as its contact area expands. Here, we examined the changes in shape, actin polymerization, focal adhesion formation and traction stress generation that accompany spreading of endothelial cells over a period of several hours. Bovine aortic endothelial cells were plated on polyacrylamide gels derivatized with a peptide containing the integrin binding sequence RGD, and changes in shape and traction force generation were measured. Notably, both the rate and extent of spreading increase with the density of substrate ligand. There are two prominent modes of spreading: at higher surface ligand densities cells tend to spread isotropically, whereas at lower densities of ligand the cells tend to anisotropically, by extending pseudopodia randomly distributed along the cell membrane. The extension of pseudopodia is followed by periods of growth in the cell body to interconnect these extensions. These cycles occur at very regular intervals and, furthermore, the extent of pseudopodial extension can be diminished by increasing the ligand density. Measurement of the traction forces exerted by the cell reveals that a cell is capable of exerting significant forces prior to either notable focal adhesion or stress fiber formation. Moreover, the total magnitude of force exerted by the cell is linearly related to the area of the cell during spreading. This study is the first to monitor the dynamic changes in the cell shape, spreading rate and the forces exerted during the early stages (first several hours) of endothelial cell adhesion.

Key Words: RGD, ecm, endothelial cells, integrin, spreading, traction stresses




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