Therapeutic Targeting of RAS Mutant Cancers
Therapeutic Targeting of RAS Mutant Cancers
Edward C. Stites, Salk Inst itute for Biological Studies, La Jolla, CA
Kendra Paskvan, Pacific Northwes t University for Health Sciences, Yakima, WA
Shumei Kato, University of California, San Diego Moores Cancer Center
Kendra Paskvan, Pacific Northwes t University for Health Sciences, Yakima, WA
Shumei Kato, University of California, San Diego Moores Cancer Center
September 2022
Paperback
9781009073646
£17.00
GBPPaperback
USD
eBook
The KRAS oncogene is believed to be the most common single nucleotide variant oncogene in human cancer. Historically, efforts to target KRAS and the other RAS GTPases have struggled. More recently, efforts have focused on identifying and exploiting features unique to specific oncogenic mutations. This has led to the first FDA approval for a RAS targeted therapy. This new agent is a covalent inhibitor that reacts with the cysteine residue created by a codon 12 glycine to cysteine (G12C) mutation within KRAS. Mutant-specific strategies may also exist for other KRAS single nucleotide variants, and recent studies provide examples and mechanisms.
Product details
September 2022Paperback
9781009073646
75 pages
228 × 152 × 3 mm
0.08kg
Available
Table of Contents
- Introduction
- RAS Biology
- Oncogenic RAS
- RAS Targeting
- Downstream Targeting
- Upstream Targeting
- Targeting Specific RAS Mutants
- KRAS G12C Targeting
- Direct Targeting of Other RAS Proteins
- KRAS G12R Pancreatic Cancer
- KRAS G13D Colorectal Cancer
- Summary
- References.
