Targeting oncogenic KRasG13C with nucleotide-based covalent inhibitors.
Lisa GoebelTonia KirschnerSandra KoskaAmrita RaiPetra JanningStefano MaffiniHelge VatheuerPaul CzodrowskiRoger S GoodyMatthias Philipp MüllerDaniel RauhPublished in: eLife (2023)
Mutations within Ras proteins represent major drivers in human cancer. In this study, we report the structure-based design, synthesis, as well as biochemical and cellular evaluation of nucleotide-based covalent inhibitors for KRasG13C, an important oncogenic mutant of Ras that has not been successfully addressed in the past. Mass spectrometry experiments and kinetic studies reveal promising molecular properties of these covalent inhibitors, and X-ray crystallographic analysis has yielded the first reported crystal structures of KRasG13C covalently locked with these GDP analogues. Importantly, KRasG13C covalently modified with these inhibitors can no longer undergo SOS-catalysed nucleotide exchange. As a final proof-of-concept, we show that in contrast to KRasG13C, the covalently locked protein is unable to induce oncogenic signalling in cells, further highlighting the possibility of using nucleotide-based inhibitors with covalent warheads in KRasG13C-driven cancer.
Keyphrases
- papillary thyroid
- endothelial cells
- induced apoptosis
- magnetic resonance
- transcription factor
- high resolution
- squamous cell carcinoma
- drug delivery
- magnetic resonance imaging
- wild type
- cell death
- molecular docking
- single molecule
- single cell
- small molecule
- contrast enhanced
- gene expression
- genome wide
- cell proliferation