MassIVE MSV000086569

Partial Public

Selective and Noncovalent Targeting of RAS Mutants for Inhibition and Degradation

Description

Activating mutants of RAS are commonly found in many human cancers, but to date selective targeting of RAS in the clinic has been limited to KRAS(G12C) through covalent inhibitors. Here, we have developed a monobody, termed 12VC1, that recognizes the active state of both KRAS(G12V) and KRAS(G12C) up to 400-times more tightly than wild-type KRAS. Affinity purification were performed on PATU8902 and H358 cell lines that contain KRAS(G12V) and KRAS(G12C), respectively, but not from growth factor stimulated HEK293T cells containing only wild-type RAS. The mass spectrometric data was acquired in data dependent mode to show the clear enrichment of KRAS in the 2 cell lines that carry the mutated RAS. In addition, a targeted analysis was performed for the peptide carrying the G12V mutation as well as the wild type KRAS peptide to further verify enrichment of only the KRAS mutant. [doi:10.25345/C5121W] [dataset license: CC0 1.0 Universal (CC0 1.0)]

Keywords: KRAS G12V ; affinity purification

Contact

Principal Investigators:
(in alphabetical order)
Beatrix Ueberheide, NYU Grossman School of Medicine, USA
Submitting User: Trixi
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