| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1996867 | Molecular Cell | 2010 | 12 Pages |
SummaryMembrane localization of the Ste11 MAPKKK is essential for activation of both the filamentous growth/invasive growth (FG/IG) MAP kinase (MAPK) pathway and the SHO1 branch of the osmoregulatory HOG MAPK pathway, and is mediated by binding of the Ste50 scaffold protein to the Opy2 membrane anchor. We found that Opy2 has two major (CR-A and CR-B), and one minor (CR-D), binding sites for Ste50. CR-A binds Ste50 constitutively and can transmit signals to both the Hog1 and Fus3/Kss1 MAPKs. CR-B, in contrast, binds Ste50 only when Opy2 is phosphorylated by Yck1/Yck2 under glucose-rich conditions and transmits the signal preferentially to the Hog1 MAPK. Ste50 phosphorylation by activated Hog1/Fus3/Kss1 MAPKs downregulates the HOG MAPK pathway by dissociating Ste50 from Opy2. Furthermore, Ste50 phosphorylation, together with MAPK-specific protein phosphatases, reduces the basal activity of the HOG and the mating MAPK pathways. Thus, dynamic regulation of Ste50-Opy2 interaction fine-tunes the MAPK signaling network.
Graphical AbstractFigure optionsDownload full-size imageDownload high-quality image (184 K)Download as PowerPoint slideHighlights► Membrane recruitment of Ste50 by Opy2 is required for HOG and FG/IG MAPK pathways ► Opy2 has two major (CR-A and CR-B), and one minor (CR-D), Ste50 binding sites ► CR-B binds Ste50 only when phosphorylated by Yck1/2 under glucose-rich conditions ► Ste50 dissociates from Opy2 when Ste50 is phosphorylated by Hog1, Fus3, or Kss1
