Discovery of Novel HPK1 Inhibitors via Chemistry-Based Direct-to-Bioassay Screening and SAR Optimization

Currently, efficient exploration of biologically relevant chemical space remains a significant challenge in lead discovery. Hematopoietic progenitor kinase 1 (HPK1) is a negative regulator of T cell activation and a high-priority target for cancer immunotherapy. Herein, we report an integrated combinatorial chemistry-biological assay approach to accelerate lead identification for HPK1. First, an in-house HPK1 inhibitor library was fragmented and recombined in silico, followed by molecular docking, yielding preferred fragments. Then, selected fragments were assembled in a microplate, and the resulting compounds were used directly to perform biological assays, leading to the identification of lead compound 8b. Guided by four series of structure–activity relationship studies, our efforts afforded the optimized compound 53 (HPK1 IC50 = 1.7 nM). Compound 53 suppressed SLP76 phosphorylation, enhanced IL-2 release in the cell, and displayed low CYP/hERG risk. Moreover, compound 53 demonstrated potent in vivo antitumor efficacy in both mouse models, which highlighted its potential as a preclinical immunotherapy candidate.