Litcius/Paper detail

Emerging strategies to target RAS signaling in human cancer therapy

Kun Chen, Yalei Zhang, Ling Qian, Peng Wang

2021Journal of Hematology & Oncology237 citationsDOIOpen Access PDF

Abstract

Abstract RAS mutations ( HRAS , NRAS , and KRAS ) are among the most common oncogenes, and around 19% of patients with cancer harbor RAS mutations. Cells harboring RAS mutations tend to undergo malignant transformation and exhibit malignant phenotypes. The mutational status of RAS correlates with the clinicopathological features of patients, such as mucinous type and poor differentiation, as well as response to anti-EGFR therapies in certain types of human cancers. Although RAS protein had been considered as a potential target for tumors with RAS mutations, it was once referred to as a undruggable target due to the consecutive failure in the discovery of RAS protein inhibitors. However, recent studies on the structure, signaling, and function of RAS have shed light on the development of RAS-targeting drugs, especially with the approval of Lumakras (sotorasib, AMG510) in treatment of KRAS G12C -mutant NSCLC patients. Therefore, here we fully review RAS mutations in human cancer and especially focus on emerging strategies that have been recently developed for RAS-targeting therapy.

Topics & Concepts

HRASKRASNeuroblastoma RAS viral oncogene homologCancer researchCancerMedicinePhenotypeMalignant transformationMutationAnti-apoptotic Ras signalling cascadeHematologyTargeted therapyInternal medicineBiologyOncologyBioinformaticsSignal transductionGeneGeneticsMAPK/ERK pathwayColorectal cancerMelanoma and MAPK PathwaysHER2/EGFR in Cancer ResearchCancer therapeutics and mechanisms