Discovery of highly potent and selective KRASG12C degraders by VHL-recruiting PROTACs for the treatment of tumors with KRASG12C-Mutation

Ning Yang; Zhiya Fan; Shiyang Sun; Xiaotong Hu; Yaqiu Mao; Changkai Jia; Xu Cai; Tingting Xu; Bingkun Li; Yi Li; Luobing Han; Ting Wei; Xiaohong Qian; Weijie Qin; Pengyun Li; Zhibing Zheng; Song Li

doi:10.1016/j.ejmech.2023.115857

Discovery of highly potent and selective KRAS^G12C degraders by VHL-recruiting PROTACs for the treatment of tumors with KRAS^G12C-Mutation

Eur J Med Chem. 2023 Dec 5:261:115857. doi: 10.1016/j.ejmech.2023.115857. Epub 2023 Oct 13.

Authors

Ning Yang¹, Zhiya Fan², Shiyang Sun¹, Xiaotong Hu¹, Yaqiu Mao¹, Changkai Jia¹, Xu Cai¹, Tingting Xu¹, Bingkun Li¹, Yi Li¹, Luobing Han¹, Ting Wei¹, Xiaohong Qian², Weijie Qin³, Pengyun Li⁴, Zhibing Zheng⁵, Song Li¹

Affiliations

¹ National Engineering Research Center for Strategic Drugs, Beijing Institute of Pharmacology and Toxicology Institution, Beijing, 100850, China.
² National Center for Protein Sciences (Beijing), Beijing Institute of Lifeomics, State Key Laboratory of Proteomics, Beijing Proteome Research Center, Beijing, 102206, China.
³ National Center for Protein Sciences (Beijing), Beijing Institute of Lifeomics, State Key Laboratory of Proteomics, Beijing Proteome Research Center, Beijing, 102206, China. Electronic address: aunp_dna@126.com.
⁴ National Engineering Research Center for Strategic Drugs, Beijing Institute of Pharmacology and Toxicology Institution, Beijing, 100850, China. Electronic address: bnuhuaxuelpy@163.com.
⁵ National Engineering Research Center for Strategic Drugs, Beijing Institute of Pharmacology and Toxicology Institution, Beijing, 100850, China. Electronic address: zzbcaptain@aliyun.com.

PMID: 37852032
DOI: 10.1016/j.ejmech.2023.115857

Abstract

Although several covalent KRAS^G12C inhibitors have made great progress in the treatment of KRAS^G12C-mutant cancer, their clinical applications are limited by adaptive resistance, motivating novel therapeutic strategies. Through drug design and structure optimization, a series of highly potent and selective KRAS^G12C Proteolysis Targeting Chimeras (PROTACs) were developed by incorporating AMG510 and VHL ligand VH032. Among them, degrader YN14 significantly inhibited KRAS^G12C-dependent cancer cells growth with nanomolar IC₅₀ and DC₅₀ values, and ＞ 95 % maximum degradation (D_max). Molecular dynamics (MD) simulation showed that YN14 induced a stable KRAS^G12C: YN14: VHL ternary complex with low binding free energy (ΔG). Notably, YN14 led to tumor regression with tumor growth inhibition (TGI%) rates more than 100 % in the MIA PaCa-2 xenograft model with well-tolerated dose-schedules. We also found that KRAS^G12C degradation exhibited advantages in overcoming adaptive KRAS^G12C feedback resistance over KRAS^G12C inhibition. Furthermore, combination of RTKs, SHP2, or CDK9 inhibitors with YN14 exhibited synergetic efficacy in KRAS^G12C-mutant cancer cells. Overall, these results demonstrated that YN14 holds exciting prospects for the treatment of tumors with KRAS^G12C-mutation and boosted efficacy could be achieved for greater clinical applications via drug combination.

Keywords: Adaptive resistance; Cancer therapy; Drug combination; KRAS(G12C); Proteolysis-targeting chimeras (PROTACs).

MeSH terms

Cytoplasm
Humans
Mutation
Neoplasms*
Proteolysis Targeting Chimera*
Proto-Oncogene Proteins p21(ras)
Von Hippel-Lindau Tumor Suppressor Protein / genetics

Substances

Proteolysis Targeting Chimera
Proto-Oncogene Proteins p21(ras)
VHL protein, human
Von Hippel-Lindau Tumor Suppressor Protein
KRAS protein, human