RAS, wanted dead or alive: Advances in targeting RAS mutant cancers
Clint A. Stalnecker, Channing J. Der
Abstract
) have the same impact on RAS signaling and function. The role of the nonmutated, wild-type RAS proteins in the context of mutant RAS is increasingly considered to be targetable, with reports of strategies that directly disrupt either the RAS interaction with activating guanine nucleotide exchange factors (GEFs) or receptor tyrosine kinase-mediated and GEF-dependent RAS activation (such as by targeting the scaffolding phosphatase SHP2). Last, the development of agents that target downstream effectors of RAS signaling has advanced substantially. In this review, we highlight some important trends in the targeting of RAS proteins in cancer.
Topics & Concepts
MutantBiologyCell biologyCancer researchComputational biologyGeneticsGeneProtein Kinase Regulation and GTPase SignalingMelanoma and MAPK PathwaysCell death mechanisms and regulation