Document Type
Article
Disciplines
Medicine and Health Sciences
Abstract
Chimaerins, a family of GTPase activating proteins (GAPs) for the small G-protein Rac, have been implicated in development, neuritogenesis, and cancer. These Rac-GAPs are regulated by the lipid second messenger diacylglycerol (DAG) generated by tyrosine-kinases such as the epidermal growth factor receptor (EGFR). Here we identify an atypical Pro-rich motif in chimaerins that binds to the adaptor protein Nck1. Unlike most Nck1 partners, chimaerins bind to the third SH3 domain of Nck1. This association is mediated by electrostatic interactions of basic residues within the Pro-rich motif with acidic clusters in the SH3 domain. EGF promotes the binding of β2-chimaerin to Nck1 in the cell periphery in a DAG-dependent manner. Moreover, β2-chimaerin translocation to the plasma membrane and its peripheral association with Rac1 requires Nck1. Our studies underscore a coordinated mechanism for β2-chimaerin activation that involves lipid interactions via the C1 domain and protein-protein interactions via the N-terminal Pro-rich region.
Recommended Citation
Mayer, Bruce J., "Coordinated Activation of the RAC-GAP β2-CHIMAERIN by an Atypical Proline-Rich Domain and Diacylglcercol" (2013). UCHC Articles - Research. 185.
https://digitalcommons.lib.uconn.edu/uchcres_articles/185
Comments
Nat Commun. Author manuscript; available in PMC 2013 July 3. Published in final edited form as: Nat Commun. 2013; 4: 1849. doi: 10.1038/ncomms2834 PMCID: PMC3700536 NIHMSID: NIHMS464427