Author:
Mesa Deborah Salvi,Barbieri Elisa,Raimondi Andrea,Freddi Stefano,Miloro Giorgia,Jendrisek Gorana,Caldieri Giusi,Quarto Micaela,Lomoriello Irene Schiano,Malabarba Maria Grazia,Bresci Arianna,Manetti Francesco,Vernuccio Federico,Abdo Hind,Scita Giorgio,Polli Dario,Tacchetti Carlo,Pinton Paolo,Bonora Massimo,Di Fiore Pier Paolo,Sigismund Sara
Abstract
AbstractOne open question in the biology of growth factor receptors is how a quantitative input (i.e.,ligand concentration) is decoded by the cell to produce specific response(s). Here, we show that an EGFR endocytic mechanism, non-clathrin endocytosis (NCE), which is activated only at high ligand concentrations and targets receptor to degradation, requires a tripartite organelle platform involving the plasma membrane (PM), endoplasmic reticulum (ER) and mitochondria. At these contact sites, EGFR-dependent, ER-generated Ca2+oscillations are sensed by mitochondria, leading to increased metabolism and ATP production. Locally released ATP is required for cortical actin remodeling and EGFR-NCE vesicle fission. The same biochemical circuitry is also needed for an effector function of EGFR, i.e., collective motility. The multiorganelle signaling platform herein described mediates direct communication between EGFR signaling and mitochondrial metabolism, and is predicted to have a broad impact on cell physiology as it is activated by another growth factor receptor, HGFR/MET.
Publisher
Cold Spring Harbor Laboratory