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. 2014 Mar 7;5:e27958. doi: 10.4161/sgtp.27958

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Copyright © 2014 Landes Bioscience

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graphic file with name sgtp-5-e27958-g2.jpg — Figure 2. Crosstalk between RhoA and Rac1 in migrating cells. At the leading edge of migrating cells, RhoA can be activated by GEFs such as p190RhoGEF, GEF-H1, LARG, and Syx. At the cell rear, RhoA can restrict Rac1 activity via FilGAP and by negatively regulating the localization of β-Pix. RhoA-stimulated mDia activity may contribute to the subsequent increase in Rac1 activity at the leading edge, possibly by activating Src-dependent GEFs such as Tiam1 and DOCK180. Rac1 can inhibit RhoA via p190RhoGAP and the decrease in RhoA activity may further activate Rac1 by preventing FilGAP activation and by relieving the inhibition of β-Pix. The association of inactive RhoA with RhoGDI could also increase Rac1 activity as a result of the competitive binding of these 2 GTPases to GDI. See text for further details.