1. Academic Validation
  2. D-1553: A novel KRASG12C inhibitor with potent and selective cellular and in vivo antitumor activity

D-1553: A novel KRASG12C inhibitor with potent and selective cellular and in vivo antitumor activity

  • Cancer Sci. 2023 May 9. doi: 10.1111/cas.15829.
Zhe Shi 1 Jifang Weng 1 Haotao Niu 1 Hong Yang 1 Rongfeng Liu 1 Yan Weng 1 Qingqing Zhu 1 Yihong Zhang 1 Liangshan Tao 1 Zhenwu Wang 1 Seok Jae Huh 2 Yueheng Jiang 1 Hong Mei 1 Xing Dai 1 Ling Zhang 1 Yaolin Wang 1
Affiliations

Affiliations

  • 1 InventisBio Co., Ltd., Shanghai, China.
  • 2 Division of Hematology-Oncology, Department of Internal Medicine, Dong-A University Hospital, Dong-A University College of Medicine, Seogu, Korea.
Abstract

D-1553 is a small molecule inhibitor selectively targeting KRASG12C and currently in phase II clinical trials. Here, we report the preclinical data demonstrating antitumor activity of D-1553. Potency and specificity of D-1553 in inhibiting GDP-bound KRASG12C mutation were determined by thermal shift assay and KRASG12C -coupled nucleotide exchange assay. In vitro and in vivo antitumor activity of D-1553 alone or in combination with other therapies were evaluated in KRASG12C mutated Cancer cells and xenograft models. D-1553 showed selective and potent activity against mutated GDP-bound KRASG12C protein. D-1553 selectively inhibited ERK phosphorylation in NCI-H358 cells harboring KRASG12C mutation. Compared to the KRAS WT and KRASG12D cell lines, D-1553 selectively inhibited cell viability in multiple KRASG12C cell lines, and the potency was slightly superior to sotorasib and adagrasib. In a panel of xenograft tumor models, D-1553, given orally, showed partial or complete tumor regression. The combination of D-1553 with chemotherapy, MEK Inhibitor, or SHP2 Inhibitor showed stronger potency on tumor growth inhibition or regression compared to D-1553 alone. These findings support the clinical evaluation of D-1553 as an efficacious drug candidate, both as a single agent or in combination, for patients with solid tumors harboring KRASG12C mutation.

Keywords

KRASG12C; inhibitor; mutation; solid tumor; targeted therapy.

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