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Novel approaches for the development of direct KRAS inhibitors: structural insights and drug design.

Kashif HaiderAnku SharmaMohammad Shahar YarPrasanna Anjaneyulu YakkalaSyed ShafiAhmed Kamal
Published in: Expert opinion on drug discovery (2022)
After the initial success in targeting the mutant KRAS G12C variants, the search has been shifted to address the challenges concerning the resistance and efficacy of small molecule KRAS inhibitors. However, the contribution of other KRAS mutations at G12V, G13C, and G13D variants causing cancers is much higher than the mutations at G12C. In view of this aspect, specific attention is required to target all other mutations as well. Accordingly, for the development of KRAS targeted therapies, the design of small molecule inhibitors that can inhibit KRAS signaling and as well as target inhibition of other signaling pathways like RAS-SOS and RAS-PI3K has to be explored extensively.
Keyphrases
  • wild type
  • small molecule
  • signaling pathway
  • copy number
  • working memory
  • young adults
  • cell proliferation
  • epithelial mesenchymal transition
  • childhood cancer