Abstract:We previously showed that guanine nucleotide-binding (G) protein α subunit (Gα)-interacting vesicle-associated protein (GIV), a guanine-nucleotide exchange factor (GEF), transactivates Gα activity-inhibiting polypeptide 1 (Gαi) proteins in response to growth factors, such as EGF, using a short C-terminal motif. Subsequent work demonstrated that GIV also binds Gαs and that inactive Gαs promotes maturation of endosomes and shuts down mitogenic MAPK–ERK1/2 signals from endosomes. However, the mechanism and conseq… Show more
“…Findings also reveal how deregulation of this pathway fuels the growth of tumor cells under energetic stress.10.7554/eLife.20795.002Figure 1.AMPK binds and phosphorylates GIV at Ser ( S ) 245.( A ) Schematic showing the functional modules of the multimodular signal transducer GIV. From the N- to the C-terminus the domains are-- a Hook-domain (grey) which binds microtubules (Simpson et al, 2005); a long coiled-coil domain (green) assists in homo/oligomerization (Enomoto et al, 2005); a Gα-binding domain (GBD; yellow) which constitutively binds Gαi/s proteins (Le-Niculescu et al, 2005); a PI(4)P-binding motif (pink) which enables GIV to bind PI4P-enriched membranes at the Golgi and the PM (Enomoto et al, 2005); an evolutionarily conserved GEF motif (red) which binds and activates Gαi (Garcia-Marcos et al, 2009) and inactivates Gαs (Gupta et al, 2016), and releases ‘free’ Gβγ from both. The C-terminal ~200 aa of GIV (purple) also has key domains that enable GIV to bind and remodel actin (Enomoto et al, 2005), bind and enhance phosphorylation of Akt (Anai et al, 2005; Enomoto et al, 2005), bind ligand-activated RTKs (Ghosh et al, 2010; Lin et al, 2014), and bind and activate Class 1 PI3-Kinases (Lin et al, 2011).…”
Loss of epithelial polarity impacts organ development and function; it is also oncogenic. AMPK, a key sensor of metabolic stress stabilizes cell-cell junctions and maintains epithelial polarity; its activation by Metformin protects the epithelial barrier against stress and suppresses tumorigenesis. How AMPK protects the epithelium remains unknown. Here, we identify GIV/Girdin as a novel effector of AMPK, whose phosphorylation at a single site is both necessary and sufficient for strengthening mammalian epithelial tight junctions and preserving cell polarity and barrier function in the face of energetic stress. Expression of an oncogenic mutant of GIV (cataloged in TCGA) that cannot be phosphorylated by AMPK increased anchorage-independent growth of tumor cells and helped these cells to evade the tumor-suppressive action of Metformin. This work defines a fundamental homeostatic mechanism by which the AMPK-GIV axis reinforces cell junctions against stress-induced collapse and also provides mechanistic insight into the tumor-suppressive action of Metformin.DOI:
http://dx.doi.org/10.7554/eLife.20795.001
“…Findings also reveal how deregulation of this pathway fuels the growth of tumor cells under energetic stress.10.7554/eLife.20795.002Figure 1.AMPK binds and phosphorylates GIV at Ser ( S ) 245.( A ) Schematic showing the functional modules of the multimodular signal transducer GIV. From the N- to the C-terminus the domains are-- a Hook-domain (grey) which binds microtubules (Simpson et al, 2005); a long coiled-coil domain (green) assists in homo/oligomerization (Enomoto et al, 2005); a Gα-binding domain (GBD; yellow) which constitutively binds Gαi/s proteins (Le-Niculescu et al, 2005); a PI(4)P-binding motif (pink) which enables GIV to bind PI4P-enriched membranes at the Golgi and the PM (Enomoto et al, 2005); an evolutionarily conserved GEF motif (red) which binds and activates Gαi (Garcia-Marcos et al, 2009) and inactivates Gαs (Gupta et al, 2016), and releases ‘free’ Gβγ from both. The C-terminal ~200 aa of GIV (purple) also has key domains that enable GIV to bind and remodel actin (Enomoto et al, 2005), bind and enhance phosphorylation of Akt (Anai et al, 2005; Enomoto et al, 2005), bind ligand-activated RTKs (Ghosh et al, 2010; Lin et al, 2014), and bind and activate Class 1 PI3-Kinases (Lin et al, 2011).…”
Loss of epithelial polarity impacts organ development and function; it is also oncogenic. AMPK, a key sensor of metabolic stress stabilizes cell-cell junctions and maintains epithelial polarity; its activation by Metformin protects the epithelial barrier against stress and suppresses tumorigenesis. How AMPK protects the epithelium remains unknown. Here, we identify GIV/Girdin as a novel effector of AMPK, whose phosphorylation at a single site is both necessary and sufficient for strengthening mammalian epithelial tight junctions and preserving cell polarity and barrier function in the face of energetic stress. Expression of an oncogenic mutant of GIV (cataloged in TCGA) that cannot be phosphorylated by AMPK increased anchorage-independent growth of tumor cells and helped these cells to evade the tumor-suppressive action of Metformin. This work defines a fundamental homeostatic mechanism by which the AMPK-GIV axis reinforces cell junctions against stress-induced collapse and also provides mechanistic insight into the tumor-suppressive action of Metformin.DOI:
http://dx.doi.org/10.7554/eLife.20795.001
“…Gupta V., et al, 15 also revealed how the pleiotropic GEF/ GDI functions of GEMs may be controlled by post-translational modifications. They showed that in the case of the prototypical GEM GIV, sequential phosphorylation of 2 Ser residues that flank the bifunctional GEF/GDI motif on GIV by 2 kinases, CDK5 35 and PKCu, 36 ensures that GIV exerts its GEF and GDI activities on Gai and Gas, respectively, in a temporally and spatially segregated manner (Fig.…”
mentioning
confidence: 99%
“…15 The members of this family share very little sequence homology and act within diverse signaling cascades; what unites them is the ability to couple activation of these cascades to G protein signaling (Fig. 1) via an evolutionarily conserved motif of »30 aa that directly binds to G proteins.…”
mentioning
confidence: 99%
“…Consequently, they all serve as nonreceptor GEFs for Gai. In the case of GIV, Gupta V., et al 15 recently demonstrated that as KB-752, GIV is a GDI for Gas 15 : it inhibits the Gas!cAMP!PKA!pCREB signaling pathway in cells using the same KB-752-like motif. These findings exposed the need for a new nomenclature, i.e., "GEM," primarily to distinguish the KB-752-like family of proteins from the other non-receptor GEFs (like Ric8A/B or AGS1) that have no propensity for pleiotropy or dual (Gai activating/Gas inhibitory) function.…”
mentioning
confidence: 99%
“…15,26 Using Gallein, 26 a compound that blocks Gbg-interactions with PI3Kg by binding to a protein-protein interaction "hot spot" on the Gb subunit, 39 it was demonstrated that the mechanism of PI3K-Akt enhancement brought about by GIV's GEM motif involves the release of 'free' Gbg-heterodimers from both Gi and Gs trimers. Because Gbg subunits interact with other components of canonical G protein signaling complexes (summarized in 40 ), e.g., receptors, Ga subunits, effectors (including GAPs and GEFs for small GTPases), and regulatory enzymes Figure 2.…”
scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.
