Rational optimization of a transcription factor activation domain inhibitor

Author:

Basu ShaonORCID,Martínez-Cristóbal Paula,Pesarrodona MireiaORCID,Frigolé-Vivas MartaORCID,Lewis Michael,Szulc Elzbieta,Bañuelos C. Adriana,Sánchez-Zarzalejo Carolina,Bielskutė StasėORCID,Zhu Jiaqi,Pombo-García Karina,Garcia-Cabau Carla,Batlle Cristina,Mateos BorjaORCID,Biesaga Mateusz,Escobedo Albert,Bardia Lídia,Verdaguer Xavier,Ruffoni Alessandro,Mawji Nasrin R.,Wang Jun,Tam Teresa,Brun-Heath Isabelle,Ventura Salvador,Meierhofer David,García Jesús,Robustelli PaulORCID,Stracker Travis H.ORCID,Sadar Marianne D.ORCID,Riera AntoniORCID,Hnisz DenesORCID,Salvatella Xavier

Abstract

SummaryTranscription factors are among the most attractive therapeutic targets but are considered largely undruggable due to the intrinsically disordered nature of their activation domains. Here we show that the aromatic character of the activation domain of the androgen receptor, a therapeutic target for castration resistant prostate cancer, is key for its activity as a transcription factor by allowing it to partition into transcriptional condensates. Based on this knowledge we optimized the structure of a small molecule inhibitor, previously identified by phenotypic screening, that targets a specific transactivation unit within the domain that is partially folded and rich in aromatic residues. The optimized compounds had more affinity for their target, inhibited androgen receptor-dependent transcriptional programs, and had antitumorigenic effect in models of castration-resistant prostate cancer in cells andin vivo. These results establish a generalizable framework to target small molecules to the activation domains of oncogenic transcription factors and other disease-associated proteins with therapeutic intent.

Publisher

Cold Spring Harbor Laboratory

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