0 citations0 references

A FAK/Src chimera with gain‐of‐function properties promotes formation of large peripheral adhesions associated with dynamic actin assembly

Cell Motility and the Cytoskeleton2007Vol. 65(1), pp. 25–39

Citations Over Time

Priscila M. F. Siesser, Leslie M. Meenderink, Larisa Ryzhova, Kristin E. Michael, David W. Dumbauld, Andrés J. Garcı́a, Irina Kaverina, Steven K. Hanks

Abstract

Formation of a complex between the tyrosine kinases FAK and Src is a key integrin-mediated signaling event implicated in cell motility, survival, and proliferation. Past studies indicate that FAK functions in the complex primarily as a "scaffold," acting to recruit and activate Src within cell/matrix adhesions. To study the cellular impact of FAK-associated Src signaling we developed a novel gain-of-function approach that involves expressing a chimeric protein with the FAK kinase domain replaced by the Src kinase domain. This FAK/Src chimera is subject to adhesion-dependent activation and promotes tyrosine phosphorylation of p130Cas and paxillin to higher steady-state levels than is achieved by wild-type FAK. When expressed in FAK -/- mouse embryo fibroblasts, the FAK/Src chimera resulted in a striking cellular phenotype characterized by unusual large peripheral adhesions, enhanced adhesive strength, and greatly reduced motility. Live cell imaging of the chimera-expressing FAK -/- cells provided evidence that the large peripheral adhesions are associated with a dynamic actin assembly process that is sensitive to a Src-selective inhibitor. These findings suggest that FAK-associated Src kinase activity has the capacity to promote adhesion integrity and actin assembly.

Citations Over Time

Abstract

Related Papers