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Cancer stem cells in personalized therapy: mechanisms, microenvironment crosstalk, and therapeutic vulnerabilities

Ling YinCenter of Disease Immunity and Intervention, College of Medicine, Lishui University, Lishui, ChinaShoubing ZhouDivision of Life Sciences and Medicine, Laboratory of Structural Immunology, Key Laboratory of Immune Response and Immunotherapy, University of Science and Technology of China, Hefei, ChinaHongliang ZhangCenter of Disease Immunity and Intervention, College of Medicine, Lishui University, Lishui, ChinaYuhua ShangAnhui Genebiol Biotech. Ltd., Hefei, ChinaSongquan WuCenter of Disease Immunity and Intervention, College of Medicine, Lishui University, Lishui, ChinaTengchuan JinAnhui Genebiol Biotech. Ltd., Hefei, China
2025en
ABI

Annotatsiya

Cancer stem cells (CSCs) drive tumor progression, therapy resistance, and metastasis through unique membrane biology, glycosylation patterns, and metabolic adaptations. CSCs exhibit a distinct glycocalyx profile enriched in hyaluronan, heparan sulfate, and sialylated glycans, facilitating immune evasion, adhesion, and survival. Key signaling pathways-Wnt/β-catenin, Hedgehog, Notch, JAK/STAT, TGF/SMAD, and PI3K/AKT/mTOR-regulate CSC stemness and therapeutic resistance. Emerging biomarkers (CD44, CD133, ALDH1, EpCAM) and targeted therapies (CAR-T cells, miRNA modulation, lipid metabolism inhibitors) show promise in disrupting CSC resilience. Advances in single-cell omics, CRISPR screening, and patient-derived organoids (PDOs) enhance CSC characterization and precision medicine applications. However, challenges remain in standardizing organoid cultures, replicating tumor microenvironments, and overcoming CSC plasticity. Integrating CSC-targeted strategies with conventional therapies may improve clinical outcomes by eradicating therapy-resistant populations and preventing relapse. This review underscores the need for innovative combination therapies to eradicate CSCs and improve clinical outcomes, while addressing challenges in biomarker validation, therapeutic resistance, and translational applications.

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