Litcius/Paper detail

Feedback activation of EGFR/wild-type RAS signaling axis limits KRASG12D inhibitor efficacy in KRASG12D-mutated colorectal cancer

Juanjuan Feng, Zhongwei Hu, Xinting Xia, Xiaogu Liu, Zhengke Lian, Hui Wang, Liren Wang, Cun Wang, Xueli Zhang, Xiufeng Pang

2023Oncogene88 citationsDOIOpen Access PDF

Abstract

Abstract Colorectal cancer (CRC), which shows a high degree of heterogeneity, is the third most deadly cancer worldwide. Mutational activation of KRAS G12D occurs in approximately 10–12% of CRC cases, but the susceptibility of KRAS G12D -mutated CRC to the recently discovered KRAS G12D inhibitor MRTX1133 has not been fully defined. Here, we report that MRTX1133 treatment caused reversible growth arrest in KRAS G12D -mutated CRC cells, accompanied by partial reactivation of RAS effector signaling. Through a drug-anchored synthetic lethality screen, we discovered that epidermal growth factor receptor (EGFR) inhibition was synthetic lethal with MRTX1133. Mechanistically, MRTX1133 treatment downregulated the expression of ERBB receptor feedback inhibitor 1 (ERRFI1), a crucial negative regulator of EGFR, thereby causing EGFR feedback activation. Notably, wild-type isoforms of RAS, including H-RAS and N-RAS, but not oncogenic K-RAS, mediated signaling downstream of activated EGFR, leading to RAS effector signaling rebound and reduced MRTX1133 efficacy. Blockade of activated EGFR with clinically used antibodies or kinase inhibitors suppressed the EGFR/wild-type RAS signaling axis, sensitized MRTX1133 monotherapy, and caused the regression of KRAS G12D -mutant CRC organoids and cell line-derived xenografts. Overall, this study uncovers feedback activation of EGFR as a prominent molecular event that restricts KRAS G12D inhibitor efficacy and establishes a potential combination therapy consisting of KRAS G12D and EGFR inhibitors for patients with KRAS G12D -mutated CRC.

Topics & Concepts

BiologyCancer researchEpidermal growth factor receptorEGFR inhibitorsColorectal cancerEffectorSignal transductionCancerERBB3KinaseImmunologyCell biologyGeneticsColorectal Cancer Treatments and StudiesChronic Lymphocytic Leukemia ResearchEnzyme Structure and Function