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Microtubules regulate GEF-H1 in response to extracellular matrix stiffness
Authors:Heck Jessica N  Ponik Suzanne M  Garcia-Mendoza Maria G  Pehlke Carolyn A  Inman David R  Eliceiri Kevin W  Keely Patricia J
Affiliation:Department of Cell and Regenerative Biology, University of Wisconsin, Madison, WI 53706, USA. heck@wisc.edu
Abstract:
Breast epithelial cells sense the stiffness of the extracellular matrix through Rho-mediated contractility. In turn, matrix stiffness regulates RhoA activity. However, the upstream signaling mechanisms are poorly defined. Here we demonstrate that the Rho exchange factor GEF-H1 mediates RhoA activation in response to extracellular matrix stiffness. We demonstrate the novel finding that microtubule stability is diminished by a stiff three-dimensional (3D) extracellular matrix, which leads to the activation of GEF-H1. Surprisingly, activation of the mitogen-activated protein kinase kinase/extracellular signal-regulated kinase pathway did not contribute to stiffness-induced GEF-H1 activation. Loss of GEF-H1 decreases cell contraction of and invasion through 3D matrices. These data support a model in which matrix stiffness regulates RhoA through microtubule destabilization and the subsequent release and activation of GEF-H1.
Keywords:
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