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SHP2 is required for growth of KRAS-mutant non-small-cell lung cancer in vivo.

Sara Mainardi ,
Antonio Mulero-Sánchez ,
Anirudh Prahallad ,
Giovanni Germano ,
Astrid Bosma ,
Paul Krimpenfort ,
Cor Lieftink ,
Jeffrey D Steinberg ,
Niels de Wit ,
Samuel Gonçalves-Ribeiro ,
Ernest Nadal ,
Alberto Bardelli ,
Alberto Villanueva ,
Rene Bernards

Abstract

RAS mutations are frequent in human cancer, especially in pancreatic, colorectal and non-small-cell lung cancers (NSCLCs)1-3. Inhibition of the RAS oncoproteins has proven difficult4, and attempts to target downstream effectors5-7 have been hampered by the activation of compensatory resistance mechanisms8. It is also well established that KRAS-mutant tumors are insensitive to inhibition of upstream growth factor receptor signaling. Thus, epidermal growth factor receptor antibody therapy is only effective in KRAS wild-type colon cancers9,10. Consistently, inhibition of SHP2 (also known as PTPN11), which links receptor tyrosine kinase signaling to the RAS-RAF-MEK-ERK pathway11,12, was shown to be ineffective in KRAS-mutant or BRAF-mutant cancer cell lines13. Our data also indicate that SHP2 inhibition in KRAS-mutant NSCLC cells under normal cell culture conditions has little effect. By contrast, SHP2 inhibition under growth factor-limiting conditions in vitro results in a senescence response. In vivo, inhibition of SHP2 in KRAS-mutant NSCLC also provokes a senescence response, which is exacerbated by MEK inhibition. Our data identify SHP2 inhibition as an unexpected vulnerability of KRAS-mutant NSCLC cells that remains undetected in cell culture and can be exploited therapeutically.

More about this publication

Nature medicine

Volume 24
Issue nr. 7
Pages 961-967
Publication date 01-07-2018

Full text links

Publisher website (DOI) 10.1038/s41591-018-0023-9
Europe PubMed Central 29808006
Pubmed 29808006

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