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. 2003 Jul;4(1):67-79.
doi: 10.1016/s1535-6108(03)00162-4.

ERK-MAPK signaling coordinately regulates activity of Rac1 and RhoA for tumor cell motility

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Free article

ERK-MAPK signaling coordinately regulates activity of Rac1 and RhoA for tumor cell motility

Emmanuel Vial et al. Cancer Cell. 2003 Jul.
Free article

Abstract

We describe two signaling events downstream of ERK-MAP kinase contributing to cell motility in colon carcinoma cells. The Fos family member Fra-1 is expressed in an ERK-dependent manner. Silencing of Fra-1 expression with short interfering RNAs leads to losses of cell polarization, motility, and invasiveness in vitro. These effects of ablating Fra-1 are a consequence of activation of a RhoA-ROCK pathway by beta1-integrin, leading to an increase in the amount of stress fibers and stabilization of focal adhesions. We propose that Fra-1 promotes cell motility by inactivating beta1-integrin and keeping RhoA activity low. This depression of RhoA activity is necessary to permit a second ERK-dependent signaling event via uPAR, the receptor for urokinase-type plasminogen activator, to activate Rac and to drive motility through polarized lamellipodia extension.

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