Inhibitor of the Nuclear Transport Protein XPO1 Enhances the Anticancer Efficacy of KRAS G12C Inhibitors in Preclinical Models of KRAS G12C-Mutant Cancers

Husain Yar Khan; Misako Nagasaka; Yiwei Li; Amro Aboukameel; Md Hafiz Uddin; Rachel Sexton; Sahar Bannoura; Yousef Mzannar; Mohammed Najeeb Al-Hallak; Steve Kim; Rafic Beydoun; Yosef Landesman; Hirva Mamdani; Dipesh Uprety; Philip A Philip; Ramzi M Mohammad; Anthony F Shields; Asfar S Azmi

doi:10.1158/2767-9764.crc-21-0176

Inhibitor of the Nuclear Transport Protein XPO1 Enhances the Anticancer Efficacy of KRAS G12C Inhibitors in Preclinical Models of KRAS G12C-Mutant Cancers

Cancer Res Commun. 2022 May;2(5):342-352. doi: 10.1158/2767-9764.crc-21-0176. Epub 2022 May 10.

Authors

Husain Yar Khan¹, Misako Nagasaka^{2

3}, Yiwei Li¹, Amro Aboukameel¹, Md Hafiz Uddin¹, Rachel Sexton¹, Sahar Bannoura¹, Yousef Mzannar¹, Mohammed Najeeb Al-Hallak¹, Steve Kim¹, Rafic Beydoun¹, Yosef Landesman⁴, Hirva Mamdani¹, Dipesh Uprety¹, Philip A Philip¹, Ramzi M Mohammad¹, Anthony F Shields¹, Asfar S Azmi¹

Affiliations

¹ Barbara Ann Karmanos Cancer Institute, Department of Oncology, Wayne State University School of Medicine, Detroit MI 48201, USA.
² University of California Irvine School of Medicine, Orange CA 92868, USA; Chao Family Comprehensive Cancer Center, Orange, CA 92868, USA.
³ Division of Neurology, Department of Internal Medicine, St. Marianna University, Kawasaki, Japan.
⁴ Karyopharm Therapeutics, Newton MA 02459, USA.

Abstract

The identification of molecules that can bind covalently to KRAS G12C and lock it in an inactive GDP-bound conformation has opened the door to targeting KRAS G12C selectively. These agents have shown promise in preclinical tumor models and clinical trials. FDA has recently granted approval to sotorasib for KRAS G12C mutated non-small cell lung cancer (NSCLC). However, patients receiving these agents as monotherapy generally develop drug resistance over time. This necessitates the development of multi-targeted approaches that can potentially sensitize tumors to KRAS inhibitors. We generated KRAS G12C inhibitor-resistant cell lines and observed that they exhibit sensitivity toward selinexor, a selective inhibitor of nuclear export protein exportin1 (XPO1), as a single agent. KRAS G12C inhibitors in combination with selinexor suppressed the proliferation of KRAS G12C mutant cancer cell lines in a synergistic manner. Moreover, combined treatment of selinexor with KRAS G12C inhibitors resulted in enhanced spheroid disintegration, reduction in the number and size of colonies formed by G12C mutant cancer cells. Mechanistically, the combination of selinexor with KRAS G12C inhibitors suppressed cell growth signaling and downregulated the expression of cell cycle markers, KRAS and NF-kB as well as increased nuclear accumulation of tumor suppressor protein Rb. In an in vivo KRAS G12C cell-derived xenograft model, oral administration of a combination of selinexor and sotorasib was demonstrated to reduce tumor burden and enhance survival. In conclusion, we have shown that the nuclear transport protein XPO1 inhibitor can enhance the anticancer activity of KRAS G12C inhibitors in preclinical cancer models.

Significance: In this study, combining nuclear transport inhibitor selinexor with KRAS G12C inhibitors has resulted in potent antitumor effects in preclinical cancer models. This can be an effective combination therapy for cancer patients that do not respond or develop resistance to KRAS G12C inhibitor treatment.

Keywords: KRAS G12C; MRTX1257; XPO1; adagrasib; selinexor; sotorasib.

Publication types

Research Support, Non-U.S. Gov't
Research Support, N.I.H., Extramural

MeSH terms

Active Transport, Cell Nucleus
Animals
Carcinoma, Non-Small-Cell Lung*
Humans
Karyopherins
Lung Neoplasms* / drug therapy
Nuclear Proteins / metabolism
Proto-Oncogene Proteins p21(ras) / genetics
Receptors, Cytoplasmic and Nuclear / genetics

Substances

Karyopherins
KRAS protein, human
Nuclear Proteins
Proto-Oncogene Proteins p21(ras)
Receptors, Cytoplasmic and Nuclear
selinexor

Grants and funding

R37 CA215427/CA/NCI NIH HHS/United States