Kinase-impaired BTK mutations are susceptible to clinical-stage BTK and IKZF1/3 degrader NX-2127.

Skye Montoya,Xiaoli Mi,Nivetha Brathaban,Vindhya Nawaratne,Stefan Gajewski,Tim Kane,Mateo Sanchez Garcia De Los Rios,Alejandro Pardo,Ratul Mukerji,Stephanie Yung,Hugo Bousquet,Carla Barrientos Risso,Hao Lu,Maurizio Affer,Anya K Sondhi,Gwenn M Hansen,Quinlan Sievers,Jordan Ye,Anthony R Mato,Omar Abdel-Wahab,Gabriel Pardo,Eric Wang,James N Iuliano,Won Jun Kim,Alexandra Chirino,Lindsey E Roeker,Ying Siow (May) Tan,Andrew D Zelenetz,Aleksandra Urban,Cristiana Guiducci,Rajesh Kumar Soni,Ryan Q Notti,Brandon Bravo,Tulasigeri M Totiger,Jessie Bourcier,Ralph Garippa,Janine Powers,Melissa Gessner,Paul Auger,Joanna M Rhodes,Adam Linley,Panga Jaipal Reddy,Mark Noviski,Camila Pena-Velasquez,Alvaro Alencar,Meghan C Thompson,Sigrid S Skånland,Sanjoy Mehta,Robert J Brown,Daniel Tsai,Justin Taylor,Cuijuan Han,Jacob Jahn

doi:10.1126/science.adi5798

Abstract

Increasing use of covalent and noncovalent inhibitors of Bruton's tyrosine kinase (BTK) has elucidated a series of acquired drug-resistant BTK mutations in patients with B cell malignancies. Here we identify inhibitor resistance mutations in BTK with distinct enzymatic activities, including some that impair BTK enzymatic activity while imparting novel protein-protein interactions that sustain B cell receptor (BCR) signaling. Furthermore, we describe a clinical-stage BTK and IKZF1/3 degrader, NX-2127, that can bind and proteasomally degrade each mutant BTK proteoform, resulting in potent blockade of BCR signaling. Treatment of chronic lymphocytic leukemia with NX-2127 achieves >80% degradation of BTK in patients and demonstrates proof-of-concept therapeutic benefit. These data reveal an oncogenic scaffold function of mutant BTK that confers resistance across clinically approved BTK inhibitors but is overcome by BTK degradation in patients.

Full Text