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Lars2-signaling mediates platinum resistance by accumulating cancer stem cell population and suppressing anti-tumor immunity.

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Drug resistance updates : reviews and commentaries in antimicrobial and anticancer chemotherapy 📖 저널 OA 3.7% 2023: 0/1 OA 2024: 0/3 OA 2025: 0/10 OA 2026: 2/40 OA 2023~2026 2026 Vol.85() p. 101330
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Wang Y, Deng M, Lei H, Miao K, Shu X, Li J

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Platinum-based chemotherapy remains a cornerstone of cancer treatment; however, its clinical efficacy is frequently compromised by acquired drug resistance.

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APA Wang Y, Deng M, et al. (2026). Lars2-signaling mediates platinum resistance by accumulating cancer stem cell population and suppressing anti-tumor immunity.. Drug resistance updates : reviews and commentaries in antimicrobial and anticancer chemotherapy, 85, 101330. https://doi.org/10.1016/j.drup.2025.101330
MLA Wang Y, et al.. "Lars2-signaling mediates platinum resistance by accumulating cancer stem cell population and suppressing anti-tumor immunity.." Drug resistance updates : reviews and commentaries in antimicrobial and anticancer chemotherapy, vol. 85, 2026, pp. 101330.
PMID 41344104 ↗

Abstract

Platinum-based chemotherapy remains a cornerstone of cancer treatment; however, its clinical efficacy is frequently compromised by acquired drug resistance. Our study elucidated a novel resistance mechanism mediated by LARS2 signaling in mammary tumors. Through comprehensive multi-omics analyses of cancer patients, mouse models, and functional validation, we demonstrated that platinum treatment upregulates LARS2 via a danger-triggered host response during resistant tumor progression, concomitant with increased chromatin accessibility. This signaling drives drug resistance through two key mechanisms: enrichment of cancer stem cells and promotion of TGF-β-mediated immunosuppression, as evidenced by M2 macrophage polarization and CD8 T cell exhaustion. Importantly, we developed an effective therapeutic strategy combining carboplatin with LARS2 signaling pathway inhibition, which successfully reversed platinum resistance and restored PD-1 checkpoint blockade sensitivity in preclinical models. These findings not only advance our understanding of chemotherapy resistance, but also provide a translatable therapeutic framework for breast cancer and other platinum-treated malignancies.

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