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Review
. 2016 Mar;94(3):253-8.
doi: 10.1007/s00109-016-1382-7. Epub 2016 Mar 9.

K-Ras protein as a drug target

Frank McCormick  1
Affiliations
Review

K-Ras protein as a drug target

Frank McCormick. J Mol Med (Berl). 2016 Mar.

Abstract

K-Ras proteins are major drivers of human cancers, playing a direct causal role in about one million cancer cases/year. In cancers driven by mutant K-Ras, the protein is locked in the active, GTP-bound state constitutively, through a defect in the off-switch mechanism. As such, the mutant protein resembles the normal K-Ras protein from a structural perspective, making therapeutic attack extremely challenging. K-Ras is a member of a large family of related proteins, which share very similar GDP/GTP-binding domains, making specific therapies more difficult. Furthermore, Ras proteins lack pockets to which small molecules can bind with high affinity, with a few interesting exceptions. However, new insights into the structure and function of K-Ras proteins reveal opportunities for intervention that were not appreciated many years ago, when efforts were launched to develop K-Ras therapies. Furthermore, K-Ras undergoes post-translational modification and interactions with cellular signaling proteins that present additional therapeutic opportunities, such as specific binding to calmodulin and regulation of non-canonical Wnt signaling.

Keywords: Cancer; K-Ras proteins; K-Ras therapies.

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Figures

Fig. 1
Fig. 1
a The Ras MAP kinase pathway. b The K-Ras 4B protein
See this image and copyright information in PMC

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