Literature DB >> 19303851

The Ste5 scaffold directs mating signaling by catalytically unlocking the Fus3 MAP kinase for activation.

Matthew Good1, Grace Tang, Julie Singleton, Attila Reményi, Wendell A Lim.   

Abstract

The scaffold protein Ste5 is required to properly direct signaling through the yeast mating pathway to the mitogen-activated protein kinase (MAPK), Fus3. Scaffolds are thought to function by tethering kinase and substrate in proximity. We find, however, that the previously identified Fus3-binding site on Ste5 is not required for signaling, suggesting an alternative mechanism controls Fus3's activation by the MAPKK Ste7. Reconstituting MAPK signaling in vitro, we find that Fus3 is an intrinsically poor substrate for Ste7, although the related filamentation MAPK, Kss1, is an excellent substrate. We identify and structurally characterize a domain in Ste5 that catalytically unlocks Fus3 for phosphorylation by Ste7. This domain selectively increases the k(cat) of Ste7-->Fus3 phosphorylation but has no effect on Ste7-->Kss1 phosphorylation. The dual requirement for both Ste7 and this Ste5 domain in Fus3 activation explains why Fus3 is selectively activated by the mating pathway and not by other pathways that also utilize Ste7.

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Year:  2009        PMID: 19303851      PMCID: PMC2777755          DOI: 10.1016/j.cell.2009.01.049

Source DB:  PubMed          Journal:  Cell        ISSN: 0092-8674            Impact factor:   41.582


  31 in total

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10.  Persistent activation by constitutive Ste7 promotes Kss1-mediated invasive growth but fails to support Fus3-dependent mating in yeast.

Authors:  Seth Maleri; Qingyuan Ge; Elizabeth A Hackett; Yuqi Wang; Henrik G Dohlman; Beverly Errede
Journal:  Mol Cell Biol       Date:  2004-10       Impact factor: 4.272

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Review 10.  Sequence patches on MAPK surfaces define protein-protein interactions.

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