Inhibition of invasion of epithelial cells by Tiam1-Rac signaling
PL Hordijk, JP Ten Klooster, RA Van Der Kammen… - Science, 1997 - science.org
PL Hordijk, JP Ten Klooster, RA Van Der Kammen, F Michiels, LCJM Oomen, JG Collard
Science, 1997•science.orgTiam1 encodes an exchange factor for the Rho-like guanosine triphosphatase Rac. Both
Tiam1 and activated RacV12 promote invasiveness of T lymphoma cells. In epithelial Madin–
Darby canine kidney (MDCK) cells, Tiam1 localized to adherens junctions. Ectopic
expression of Tiam1 or RacV12 inhibited hepatocyte growth factor–induced scattering by
increasing E-cadherin–mediated cell-cell adhesion accompanied by actin polymerization at
cell-cell contacts. In Ras-transformed MDCK cells, expression of Tiam1 or RacV12 restored …
Tiam1 and activated RacV12 promote invasiveness of T lymphoma cells. In epithelial Madin–
Darby canine kidney (MDCK) cells, Tiam1 localized to adherens junctions. Ectopic
expression of Tiam1 or RacV12 inhibited hepatocyte growth factor–induced scattering by
increasing E-cadherin–mediated cell-cell adhesion accompanied by actin polymerization at
cell-cell contacts. In Ras-transformed MDCK cells, expression of Tiam1 or RacV12 restored …
Tiam1 encodes an exchange factor for the Rho-like guanosine triphosphatase Rac. Both Tiam1 and activated RacV12 promote invasiveness of T lymphoma cells. In epithelial Madin–Darby canine kidney (MDCK) cells, Tiam1 localized to adherens junctions. Ectopic expression of Tiam1 or RacV12 inhibited hepatocyte growth factor–induced scattering by increasing E-cadherin–mediated cell-cell adhesion accompanied by actin polymerization at cell-cell contacts. In Ras-transformed MDCK cells, expression of Tiam1 or RacV12 restored E-cadherin–mediated adhesion, resulting in phenotypic reversion and loss of invasiveness. These data suggest an invasion-suppressor role for Tiam1 and Rac in epithelial cells.
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