Domain-specific p53 mutants activate EGFR by distinct mechanisms exposing tissue-independent therapeutic vulnerabilities.
Teresa Lai Fong HoMay Yin LeeHui Chin GohGermaine Yi Ning NgJane Jia Hui LeeSrinivasaraghavan KannanYan Ting LimTianyun ZhaoEdwin Kok Hao LimCheryl Zi Jin PhuaYi Fei LeeRebecca Yi Xuan LimPerry Jun Hao NgJu YuanDedrick Kok Hong ChanBettina LieskeChoon Seng ChongKuok Chung LeeJeffrey Hy LumWai Kit CheongKhay-Guan YeohKer Kan TanRadoslaw Mikolaj SobotaChandra S VermaDavid P LaneWai Leong TamAshok R VenkitaramanPublished in: Nature communications (2023)
Mis-sense mutations affecting TP53 promote carcinogenesis both by inactivating tumor suppression, and by conferring pro-carcinogenic activities. We report here that p53 DNA-binding domain (DBD) and transactivation domain (TAD) mis-sense mutants unexpectedly activate pro-carcinogenic epidermal growth factor receptor (EGFR) signaling via distinct, previously unrecognized molecular mechanisms. DBD- and TAD-specific TP53 mutants exhibited different cellular localization and induced distinct gene expression profiles. In multiple tissues, EGFR is stabilized by TAD and DBD mutants in the cytosolic and nuclear compartments respectively. TAD mutants promote EGFR-mediated signaling by enhancing EGFR interaction with AKT via DDX31 in the cytosol. Conversely, DBD mutants maintain EGFR activity in the nucleus, by blocking EGFR interaction with the phosphatase SHP1, triggering c-Myc and Cyclin D1 upregulation. Our findings suggest that p53 mutants carrying gain-of-function, mis-sense mutations affecting two different domains form new protein complexes that promote carcinogenesis by enhancing EGFR signaling via distinctive mechanisms, exposing clinically relevant therapeutic vulnerabilities.