SHOC2 phosphatase-dependent RAF dimerization mediates resistance to MEK inhibition in RAS-mutant cancers.
Greg G JonesIsabel Boned Del RíoSibel SariAysen SekerimLucy C YoungNicole HartigItziar Areso ZubiaurMona A El-BahrawyRobert Edward HyndsWinnie LeiMiriam Molina-ArcasJulian DownwardPablo Rodriguez-VicianaPublished in: Nature communications (2019)
Targeted inhibition of the ERK-MAPK pathway, upregulated in a majority of human cancers, has been hindered in the clinic by drug resistance and toxicity. The MRAS-SHOC2-PP1 (SHOC2 phosphatase) complex plays a key role in RAF-ERK pathway activation by dephosphorylating a critical inhibitory site on RAF kinases. Here we show that genetic inhibition of SHOC2 suppresses tumorigenic growth in a subset of KRAS-mutant NSCLC cell lines and prominently inhibits tumour development in autochthonous murine KRAS-driven lung cancer models. On the other hand, systemic SHOC2 ablation in adult mice is relatively well tolerated. Furthermore, we show that SHOC2 deletion selectively sensitizes KRAS- and EGFR-mutant NSCLC cells to MEK inhibitors. Mechanistically, SHOC2 deletion prevents MEKi-induced RAF dimerization, leading to more potent and durable ERK pathway suppression that promotes BIM-dependent apoptosis. These results present a rationale for the generation of SHOC2 phosphatase targeted therapies, both as a monotherapy and to widen the therapeutic index of MEK inhibitors.
Keyphrases
- wild type
- pi k akt
- signaling pathway
- cell cycle arrest
- small cell lung cancer
- induced apoptosis
- oxidative stress
- cell proliferation
- endoplasmic reticulum stress
- randomized controlled trial
- endothelial cells
- primary care
- clinical trial
- genome wide
- metabolic syndrome
- open label
- type diabetes
- advanced non small cell lung cancer
- cell death
- adipose tissue
- atrial fibrillation
- dna methylation
- drug induced
- young adults
- tyrosine kinase
- cancer therapy
- study protocol
- anti inflammatory
- combination therapy
- childhood cancer
- catheter ablation
- stress induced