Determining the ERK-regulated phosphoproteome driving KRAS-mutant cancer.
Jennifer E KlompJ Nathaniel DiehlJeffrey A KlompA Cole EdwardsRunying YangAlexis J MoralesKhalilah E TaylorKristina Drizyte-MillerKirsten L BryantAntje SchaeferJared L JohnsonEmily M HuntsmanTomer M YaronMariaelena PierobonElisa BaldelliAlex W PrevatteNatalie K BarkerLaura E HerringEmanuel F PetricoinLee M GravesLewis C CantleyAdrienne D CoxChanning J DerClint A StalneckerPublished in: Science (New York, N.Y.) (2024)
To delineate the mechanisms by which the ERK1 and ERK2 mitogen-activated protein kinases support mutant KRAS-driven cancer growth, we determined the ERK-dependent phosphoproteome in KRAS-mutant pancreatic cancer. We determined that ERK1 and ERK2 share near-identical signaling and transforming outputs and that the KRAS-regulated phosphoproteome is driven nearly completely by ERK. We identified 4666 ERK-dependent phosphosites on 2123 proteins, of which 79 and 66%, respectively, were not previously associated with ERK, substantially expanding the depth and breadth of ERK-dependent phosphorylation events and revealing a considerably more complex function for ERK in cancer. We established that ERK controls a highly dynamic and complex phosphoproteome that converges on cyclin-dependent kinase regulation and RAS homolog guanosine triphosphatase function (RHO GTPase). Our findings establish the most comprehensive molecular portrait and mechanisms by which ERK drives KRAS-dependent pancreatic cancer growth.