Direct and selective pharmacological disruption of the YAP-TEAD interface by IAG933 inhibits Hippo-dependent and RAS-MAPK-altered cancers

Emilie A Chapeau; Laurent Sansregret; Giorgio G Galli; Patrick Chène; Markus Wartmann; Thanos P Mourikis; Patricia Jaaks; Sabrina Baltschukat; Ines A M Barbosa; Daniel Bauer; Saskia M Brachmann; Clara Delaunay; Claire Estadieu; Jason E Faris; Pascal Furet; Stefanie Harlfinger; Andreas Hueber; Eloísa Jiménez Núñez; David P Kodack; Emeline Mandon; Typhaine Martin; Yannick Mesrouze; Vincent Romanet; Clemens Scheufler; Holger Sellner; Christelle Stamm; Dario Sterker; Luca Tordella; Francesco Hofmann; Nicolas Soldermann; Tobias Schmelzle

doi:10.1038/s43018-024-00754-9

Direct and selective pharmacological disruption of the YAP-TEAD interface by IAG933 inhibits Hippo-dependent and RAS-MAPK-altered cancers

Nat Cancer. 2024 Jul;5(7):1102-1120. doi: 10.1038/s43018-024-00754-9. Epub 2024 Apr 2.

Authors

Emilie A Chapeau¹, Laurent Sansregret², Giorgio G Galli², Patrick Chène², Markus Wartmann², Thanos P Mourikis², Patricia Jaaks², Sabrina Baltschukat², Ines A M Barbosa², Daniel Bauer², Saskia M Brachmann², Clara Delaunay², Claire Estadieu², Jason E Faris³, Pascal Furet², Stefanie Harlfinger^{2

4}, Andreas Hueber², Eloísa Jiménez Núñez², David P Kodack³, Emeline Mandon², Typhaine Martin², Yannick Mesrouze², Vincent Romanet², Clemens Scheufler², Holger Sellner², Christelle Stamm², Dario Sterker², Luca Tordella², Francesco Hofmann^{2

5}, Nicolas Soldermann², Tobias Schmelzle⁶

Affiliations

¹ Novartis BioMedical Research, Basel, Switzerland. [email protected].
² Novartis BioMedical Research, Basel, Switzerland.
³ Novartis BioMedical Research, Cambridge, MA, USA.
⁴ AstraZeneca, Oncology R&D, Cambridge, UK.
⁵ Pierre Fabre Group, R&D Medical Care, Toulouse, France.
⁶ Novartis BioMedical Research, Basel, Switzerland. [email protected].

Abstract

The YAP-TEAD protein-protein interaction mediates YAP oncogenic functions downstream of the Hippo pathway. To date, available YAP-TEAD pharmacologic agents bind into the lipid pocket of TEAD, targeting the interaction indirectly via allosteric changes. However, the consequences of a direct pharmacological disruption of the interface between YAP and TEADs remain largely unexplored. Here, we present IAG933 and its analogs as potent first-in-class and selective disruptors of the YAP-TEAD protein-protein interaction with suitable properties to enter clinical trials. Pharmacologic abrogation of the interaction with all four TEAD paralogs resulted in YAP eviction from chromatin and reduced Hippo-mediated transcription and induction of cell death. In vivo, deep tumor regression was observed in Hippo-driven mesothelioma xenografts at tolerated doses in animal models as well as in Hippo-altered cancer models outside mesothelioma. Importantly this also extended to larger tumor indications, such as lung, pancreatic and colorectal cancer, in combination with RTK, KRAS-mutant selective and MAPK inhibitors, leading to more efficacious and durable responses. Clinical evaluation of IAG933 is underway.

MeSH terms

Adaptor Proteins, Signal Transducing / metabolism
Animals
Antineoplastic Agents / pharmacology
Antineoplastic Agents / therapeutic use
Cell Line, Tumor
DNA-Binding Proteins / metabolism
Female
Hippo Signaling Pathway*
Humans
Mice
Neoplasms / drug therapy
Neoplasms / metabolism
Protein Serine-Threonine Kinases* / metabolism
Signal Transduction / drug effects
TEA Domain Transcription Factors
Transcription Factors* / metabolism
Xenograft Model Antitumor Assays*
YAP-Signaling Proteins / metabolism
ras Proteins / metabolism

Substances

Transcription Factors
Protein Serine-Threonine Kinases
Adaptor Proteins, Signal Transducing
YAP-Signaling Proteins
YAP1 protein, human
DNA-Binding Proteins
TEA Domain Transcription Factors
ras Proteins
Antineoplastic Agents