Article Synopsis
- Mutations in Ras proteins are found in 33% of human cancers, making them difficult to target directly with drugs.
- Researchers discovered a compound called 249C that specifically targets Ras-mutant cancer cells, showing strong effectiveness in the nanomolar range.
- 249C works by inhibiting the activity of a protein called V-ATPase, leading to disrupted cellular processes essential for Ras-driven cancers, with particularly strong effects on tumors with KRASG13D and G12V mutations.
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Article Abstract
Mutations in Ras family proteins are implicated in 33% of human cancers, but direct pharmacological inhibition of Ras mutants remains challenging. As an alternative to direct inhibition, we screened for sensitivities in Ras-mutant cells and discovered 249C as a Ras-mutant selective cytotoxic agent with nanomolar potency against a spectrum of Ras-mutant cancers. 249C binds to vacuolar (V)-ATPase with nanomolar affinity and inhibits its activity, preventing lysosomal acidification and inhibiting autophagy and macropinocytosis pathways that several Ras-driven cancers rely on for survival. Unexpectedly, potency of 249C varies with the identity of the Ras driver mutation, with the highest potency for KRASG13D and G12V both in vitro and in vivo, highlighting a mutant-specific dependence on macropinocytosis and lysosomal pH. Indeed, 249C potently inhibits tumor growth without adverse side effects in mouse xenografts of KRAS-driven lung and colon cancers. A comparison of isogenic SW48 xenografts with different KRAS mutations confirmed that KRASG13D/+ (followed by G12V/+) mutations are especially sensitive to 249C treatment. These data establish proof-of-concept for targeting V-ATPase in cancers driven by specific KRAS mutations such as KRASG13D and G12V.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9750872 | PMC |
| http://dx.doi.org/10.1038/s41587-022-01386-z | DOI Listing |
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