Article
- The EMBO Journal (2004) 23, 3492 - 3504
- doi:10.1038/sj.emboj.7600331
Published online: 12 August 2004
Subject Category:
Novel regulatory mechanisms for the Dbl family guanine nucleotide exchange factor Cool-2/
-Pix
Qiyu Feng1,2, Daniel Baird1,2 and Richard A Cerione1,2
- Department of Molecular Medicine, Cornell University, Ithaca, NY, USA
- Department of Chemistry and Chemical Biology, Cornell University, Ithaca, NY, USA
Correspondence to:
Richard A Cerione, Department of Molecular Medicine, College of Veterinary Medicine, Cornell University, Veterinary Medical Center C3-155, Ithaca, NY 14853-6401, USA. Tel.: +1 607 253 3650/3888; Fax: +1 607 253 3659; E-mail: rac1@cornell.edu
Received 26 April 2004; Accepted 24 June 2004
Abstract
The Cool-2 (cloned-out of library-2) protein (identical to
-Pix for Pak-interactive exchange factor) has been implicated in various biological responses including chemoattractant signaling and in certain forms of mental retardation. We show that when Cool-2 exists as a dimer, it functions as a Rac-specific guanine nucleotide exchange factor (GEF). Dimerization of Cool-2 enables its Dbl (diffuse B-cell lymphoma) and pleckstrin homology domains to work together (in trans) to bind specifically to Rac-GDP. Dissociation of dimeric Cool-2 into its monomeric form allows it to act as a GEF for Cdc42 as well as for Rac. The binding of either PAK (p21-activated kinase) or Cbl (Casitas B-lymphoma) to the SH3 domain of monomeric Cool-2 is necessary for the functional interactions between GDP-bound Cdc42 or Rac and the Cool-2 monomer. The 
subunit complex of large GTP-binding proteins, by interacting with PAK, stimulates the dissociation of the Cool-2 dimer and activates its GEF activity for Cdc42. Overall, these findings highlight novel mechanisms by which extracellular signals can direct the specific activation of Rac versus Cdc42 by Cool-2/
-Pix.
Keywords:
- Cdc42,
- Cool,
- Pix,
- Rac,
- signaling
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