Peng Jingjing, Ding Xiaoyu, Chen Celia Xiaojing, Zhao Pei, Ding Xiao, Zhang Man, Aliper Alex, Ren Feng, Lu Hongfu, Zhavoronkov Alex
Insilico Medicine Shanghai Ltd, Suite 901, Tower C, Changtai Plaza, 2889 Jinke Road, Pudong New District, Shanghai 201203, China.
Insilico Medicine AI Limited, Masdar City, Abu Dhabi 145748, UAE.
J Med Chem. 2024 Dec 12;67(23):21520-21544. doi: 10.1021/acs.jmedchem.4c02421. Epub 2024 Nov 25.
Hematopoietic progenitor kinase 1 (HPK1) has emerged as an attractive target for immunotherapy due to its critical role in T cell activation and proliferation. The major challenge in developing HPK1 inhibitors lies in balancing kinase selectivity, pharmacokinetic (PK) properties, and therapeutic efficacy. In this study, we report a series of pyridine-2-carboxamide analogues demonstrating strong HPK1 inhibitory activity in enzymatic and cellular assays, along with good kinase selectivity. Among these analogues, compound showed good in vitro HPK1 inhibitory activity, excellent kinase selectivity (>637-fold vs GCK-like kinase and >1022-fold vs LCK), and robust in vivo efficacy in the CT26 (tumor growth inhibition (TGI) = 94.3%, 2/6 CRs) and MC38 murine colorectal cancer models (TGI = 83.3%, 1/6 complete response) when administered in combination with anti-PD-1. Compound also demonstrated adequate in vitro ADME and in vivo PK properties, displaying good oral bioavailability across multiple species ( % = 35-63). These findings summarize our compound's favorable safety and efficacy profiles, justifying its testing in future translational studies.
造血祖细胞激酶1(HPK1)因其在T细胞活化和增殖中的关键作用,已成为免疫治疗的一个有吸引力的靶点。开发HPK1抑制剂的主要挑战在于平衡激酶选择性、药代动力学(PK)特性和治疗效果。在本研究中,我们报告了一系列吡啶-2-甲酰胺类似物,它们在酶学和细胞试验中表现出强大的HPK1抑制活性,以及良好的激酶选择性。在这些类似物中,化合物 在体外表现出良好的HPK1抑制活性、出色的激酶选择性(与GCK样激酶相比>637倍,与LCK相比>1022倍),并且在与抗PD-1联合给药时,在CT26(肿瘤生长抑制(TGI)=94.3%,2/6完全缓解)和MC38小鼠结直肠癌模型中具有强大的体内疗效(TGI = 83.3%,1/6完全缓解)。化合物 还表现出足够的体外ADME和体内PK特性,在多个物种中显示出良好的口服生物利用度(% = 35-63)。这些发现总结了我们化合物良好的安全性和疗效概况,证明了其在未来转化研究中的测试价值。
