p53 activation enhances the sensitivity of non-small cell lung cancer to the combination of SH003 and docetaxel by inhibiting de novo pyrimidine synthesis

Yu-Jeong Choi; Kangwook Lee; Seo Yeon Lee; Youngbin Kwon; Jaehyuk Woo; Chan-Yong Jeon; Seong-Gyu Ko

doi:10.1186/s12935-024-03337-x

Cancer Cell International (May 2024)

p53 activation enhances the sensitivity of non-small cell lung cancer to the combination of SH003 and docetaxel by inhibiting de novo pyrimidine synthesis

Yu-Jeong Choi,
Kangwook Lee,
Seo Yeon Lee,
Youngbin Kwon,
Jaehyuk Woo,
Chan-Yong Jeon,
Seong-Gyu Ko

Affiliations

Yu-Jeong Choi: Department of Preventive Medicine, College of Korean Medicine, Kyung Hee University
Kangwook Lee: Department of Food and Biotechnology, Korea University
Seo Yeon Lee: Department of Internal Medicine, Yale University
Youngbin Kwon: Department of Korean Medicine, Graduate School, Kyung Hee University
Jaehyuk Woo: Department of Korean Medicine, Graduate School, Kyung Hee University
Chan-Yong Jeon: Department of Internal Medicine, College of Korean Medicine, Gachon University
Seong-Gyu Ko: Department of Preventive Medicine, College of Korean Medicine, Kyung Hee University

DOI: https://doi.org/10.1186/s12935-024-03337-x
Journal volume & issue: Vol. 24, no. 1
pp. 1 – 13

Abstract

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Abstract Background Identifying molecular biomarkers for predicting responses to anti-cancer drugs can enhance treatment precision and minimize side effects. This study investigated the novel cancer-targeting mechanism of combining SH003, an herbal medicine, with docetaxel in non-small cell lung cancer (NSCLC) cells. Also, the present study aimed to identify the genetic characteristics of cancer cells susceptible to this combination. Methods Cell viability was analyzed by WST-8 assay. Apoptosis induction, BrdU incorporation, and cell cycle analysis were performed using flow cytometry. Metabolites were measured by LC–MS/MS analysis. Real-time PCR and western blotting evaluated RNA and protein expression. DNA damage was quantified through immunofluorescence. cBioPortal and GEPIA data were utilized to explore the mutual co-occurrence of TP53 and UMPS and UMPS gene expression in NSCLC. Results The combination treatment suppressed de novo pyrimidine nucleotide biosynthesis by reducing the expression of related enzymes. This blockade of pyrimidine metabolism led to DNA damage and subsequent apoptosis, revealing a novel mechanism for inducing lung cancer cell death with this combination. However, some lung cancer cells exhibited distinct responses to the combination treatment that inhibited pyrimidine metabolism. The differences in sensitivity in lung cancer cells were determined by the TP53 gene status. TP53 wild-type lung cancer cells were effectively inhibited by the combination treatment through p53 activation, while TP53 mutant- or null-type cells exhibited lower sensitivity. Conclusions This study, for the first time, established a link between cancer cell genetic features and treatment response to simultaneous SH003 and docetaxel treatment. It highlights the significance of p53 as a predictive factor for susceptibility to this combination treatment. These findings also suggest that p53 status could serve as a crucial criterion in selecting appropriate therapeutic strategies for targeting pyrimidine metabolism in lung cancer.

Published in Cancer Cell International

ISSN: 1475-2867 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens; Science: Biology (General): Cytology
Website: https://cancerci.biomedcentral.com

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