An allosteric pan-TEAD inhibitor blocks oncogenic YAP/TAZ signaling and overcomes KRAS G12C inhibitor resistance.
Thijs J HagenbeekJason R ZbiegMarc HafnerRana MroueJennifer A LacapNicole M SodirCameron L NolandShervin AfghaniAyush KishoreKamakoti P BhatXiaosai YaoStephen SchmidtSaundra ClausenMicah SteffekWendy LeePaul BerozaScott MartinEva LinRina FongPaola Di LelloMarta H KubalaMichelle N-Y YangJeffrey T LauEmily ChanAlfonso ArrazateLe AnElizabeth LevyMaria N LorenzoHo-June LeeTrang H PhamZora ModrusanRichard ZangYi-Chen ChenMichal KabzaMusaddeque AhmedJason LiMatthew T ChangDanilo MaddaloMarie EvangelistaXin YeJames J CrawfordAnwesha DeyPublished in: Nature cancer (2023)
The Hippo pathway is a key growth control pathway that is conserved across species. The downstream effectors of the Hippo pathway, YAP (Yes-associated protein) and TAZ (transcriptional coactivator with PDZ-binding motif), are frequently activated in cancers to drive proliferation and survival. Based on the premise that sustained interactions between YAP/TAZ and TEADs (transcriptional enhanced associate domain) are central to their transcriptional activities, we discovered a potent small-molecule inhibitor (SMI), GNE-7883, that allosterically blocks the interactions between YAP/TAZ and all human TEAD paralogs through binding to the TEAD lipid pocket. GNE-7883 effectively reduces chromatin accessibility specifically at TEAD motifs, suppresses cell proliferation in a variety of cell line models and achieves strong antitumor efficacy in vivo. Furthermore, we uncovered that GNE-7883 effectively overcomes both intrinsic and acquired resistance to KRAS (Kirsten rat sarcoma viral oncogene homolog) G12C inhibitors in diverse preclinical models through the inhibition of YAP/TAZ activation. Taken together, this work demonstrates the activities of TEAD SMIs in YAP/TAZ-dependent cancers and highlights their potential broad applications in precision oncology and therapy resistance.
Keyphrases