PO.CL05.10 · 临床研究
Efficacy, in vivo safety, and PK/PD studies for novel, oral, highly selective PTPN2/1 inhibitor (ZE00-0388)
作者与单位
摘要 Abstract
PTPN2 inhibition is a novel immuno-oncology approach: by releasing an intracellular “brake” it increases cytokine responsiveness (e.g., IFN-gamma/JAK-STAT), boosts antigen presentation, and enhances T-cell cytotoxicity, helping to overcome immune evasion in tumors resistant to PD-1 blockade.
Our development candidate ZE00-0388 demonstrates potential best-in-class profile: Nanomolar potency with high selectivity for PTPN2/1 over other phosphatases, predictable PK/PD with sustained exposure above EC50, and proven target engagement. ZE00-0388 shows favorable bioavailability in all species, with best translation expected from dog to human.
The combination of anti-mPD-1 and ZE00-0388 exhibited remarkable dose-dependent anti-tumor efficacy against the subcutaneous MC38 colon model. Solo treatments with ZE00-0388 demonstrated tumor growth inhibition of 81% and in combination with anti-mPD-1 complete regression of tumor in 50% of animals. ZE00-0388 has a very favorable safety profile with tolerated doses significantly above pre-clinical proof-of-concept efficacious doses, which indicates that ZE00-0388 should have a very broad therapeutic window.
利益披露 Disclosure
A. Pushechnikov, None..
R. Karapetian, None..
S. Mochalov, None..
S. Baumann Tomovska, None..
N. Savchuk, None..
I. Dukes, None..
R. Abagyan, None.