PO.CH01.03 · 化学
Discovery and preclinical evaluation of a potent, orally bioavailable, highly selective, small molecule non-covalent KRAS[G12D] inhibitor
作者与单位
摘要 Abstract
KRAS[G12D] oncogenic mutation is present in ~35% of pancreatic, 13% of colorectal, and 4% of non-small cell lung cancers. The mutation also occurs in other cancer types, albeit less frequently. Here we would like to present compelling evidences that ZE98-0277 has potent and selective activity in KRAS[G12D] mutant cell lines and in vivo models.
ZE98-0277 drug candidate demonstrates strong in vitro activity (IC50 KRAS[G12D] 6.3 nM) and oral PK, bioavailability ~20-40% in mice and monkeys, broad therapeutic window (>100x in cellular models), good safety and tolerability, favorable ADME properties (solubility, stability, permeability, low hERG inhibition, minimal off-target effects), effective tumor suppression in multiple mouse xenograft models.
These preclinical results demonstrate that ZE98-0277 is a potent, selective, and orally bioavailable KRAS[G12D] inhibitor, strongly efficacious against KRAS[G12D] mutant tumors slated for further development.
利益披露 Disclosure
A. Pushechnikov, None..
V. Kysil, None..
R. Karapetian, None..
S. Mochalov, None..
A. Riakhovskii, None..
E. Bulanova, None..
N. Savchuk, None..
I. Dukes, None.