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Repurposing of the Macrolide Antibiotic Clarithromycin for the Prevention of Lung Cancer.

Molecular cancer therapeutics 2026 Vol.25(2) p. 283-294

Deng S, Hussain T, Bartelli TF, Sebastian MM, Zarghooni M, Velasco WV, Somerville B, Phan L, Savage MI, Song Y, Clifford JL, Kadara H, McAllister F, Brown PH, Moghaddam SJ, Aldaz CM

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Drug repurposing is the process of reusing existing pharmaceuticals for novel clinical purposes, which offers advantages such as streamlined clinical trial access and reduced drug development costs.

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APA Deng S, Hussain T, et al. (2026). Repurposing of the Macrolide Antibiotic Clarithromycin for the Prevention of Lung Cancer.. Molecular cancer therapeutics, 25(2), 283-294. https://doi.org/10.1158/1535-7163.MCT-25-0392
MLA Deng S, et al.. "Repurposing of the Macrolide Antibiotic Clarithromycin for the Prevention of Lung Cancer.." Molecular cancer therapeutics, vol. 25, no. 2, 2026, pp. 283-294.
PMID 41024580

Abstract

Drug repurposing is the process of reusing existing pharmaceuticals for novel clinical purposes, which offers advantages such as streamlined clinical trial access and reduced drug development costs. Clarithromycin (CAM), a member of the macrolide antibiotics family, is a promising candidate for repurposing in cancer therapy due to its known preclinical and clinical immunomodulatory and anticancer properties. In the current study, we investigated whether CAM could be repurposed as a preventive treatment for KRAS-mutant lung cancer, a subtype of lung adenocarcinoma that is strongly associated with heavy smoking. CCSPCre; LSL-KrasG12D mice at an early stage of tumor development were treated with different doses of CAM for 10 weeks. While exhibiting an excellent safety profile, CAM was able to prevent the development of premalignant and malignant lung lesions in a dose-dependent manner. In addition, CAM significantly reduced the infiltration of neutrophils/polymorphonuclear myeloid-derived suppressor cells and inhibited the mRNA expression of protumor inflammatory cytokines IL-6, TNFα, and IL-1β, as well as M2 macrophage markers Fizz1 and Arginase1 in the lung tumor microenvironment. Moreover, we investigated the effect of CAM in reshaping the intestinal and lung microbiome. Long-term CAM usage decreased intestinal microbiome diversity but, more notably, significantly increased the abundance of the probiotic genus Muribaculaceae while decreasing the abundance of Desulfovibrio, a genus associated with the promotion of various malignancies. Taken together, we conclude that CAM could provide promising cancer prevention efficacy in KRAS-mutant lung cancer due to its immunomodulatory properties on the tumor microenvironment and its regulatory effects on the microbiome.

MeSH Terms

Animals; Lung Neoplasms; Mice; Clarithromycin; Drug Repositioning; Anti-Bacterial Agents; Humans; Tumor Microenvironment

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