EGFR inhibitor suppresses tumor growth by blocking lipid uptake and cholesterol synthesis in non-small cell lung cancer
- Authors
- Rhie, Byung-Ho; Woo, Sang Hyeon; Kim, Hyun-Yi; Karapurkar, Janardhan Keshav; Jo, Won-Jun; Kim, Jusong; Kim, Dong Ha; Kim, Jaesang; Choi, Myeong Jun; Park, Young Jun; Hong, Yoonki; Hong, Seok-Ho; Ramakrishna, Suresh; Kim, Kye-Seong
- Issue Date
- Oct-2025
- Publisher
- Elsevier BV
- Keywords
- Cholesterol biosynthesis; Epidermal growth factor receptor; Kinase activity; Lipid uptake; Low-density lipoprotein receptor; Non-small cell lung cancer; Tumor growth
- Citation
- Biochimica et Biophysica Acta (BBA) - Molecular Basis of Disease, v.1871, no.7, pp 1 - 11
- Pages
- 11
- Indexed
- SCIE
SCOPUS
- Journal Title
- Biochimica et Biophysica Acta (BBA) - Molecular Basis of Disease
- Volume
- 1871
- Number
- 7
- Start Page
- 1
- End Page
- 11
- URI
- https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/208567
- DOI
- 10.1016/j.bbadis.2025.167957
- ISSN
- 0925-4439
1879-260X
- Abstract
- Accelerated cholesterol and lipid metabolism are hallmarks of non-small cell lung cancer (NSCLC). Recently, epidermal growth factor receptor (EGFR) signaling has been shown to regulate de novo cholesterol synthesis and low-density lipoprotein receptor (LDLR) expression through SREBP-1-dependent pathways. This suggests that targeting EGFR signaling in cholesterol metabolism might provide a new therapeutic strategy for NSCLC. In this study, we demonstrated that AX-0085, a small-molecule drug, significantly inhibits EGFR kinase activity and subsequently suppresses cholesterol and lipid metabolism in NSCLC. Transcriptomic analysis showed that cholesterol and lipid metabolism-related transcripts were significantly downregulated in AX-0085-treated NSCLC cells compared to the mock control. In addition, AX-0085 downregulates EGF signaling-dependent SREBP1-mediated cholesterol biosynthesis-related enzymes and LDLR in NSCLC. Moreover, AX-0085 dramatically reduced proliferation, colony-forming ability, and migration in NSCLC cells by blocking EGFR signaling. Furthermore, treatment with AX-0085 decreased both tumor size and volume in the LLC-xenograft model. These results demonstrate that AX-0085 effectively suppresses cholesterol metabolism in NSCLC cells by inhibiting EGF-mediated SREBP1 signaling, suggesting a potential therapeutic strategy targeting cholesterol metabolism in NSCLC.
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