Department of Microbiology and Immunology, School of Dentistry, Kyungpook National University, Daegu 700-412, Korea.
Department of Oral Pathology, School of Dentistry, Kyungpook National University, Daegu 700-412, Korea.
Theranostics. 2024 Jan 1;14(2):460-479. doi: 10.7150/thno.87329. eCollection 2024.
Platinum-based chemotherapy is commonly used for treating solid tumors, but drug resistance often limits its effectiveness. Cancer-associated fibroblast (CAF)-derived extracellular vesicle (EV), which carry various miRNAs, have been implicated in chemotherapy resistance. However, the molecular mechanism through which CAFs modulate cisplatin resistance in oral squamous cell carcinoma (OSCC) is not well understood. We employed two distinct primary CAF types with differential impacts on cancer progression: CAF-P, representing a more aggressive cancer-promoting category, and CAF-D, characterized by properties that moderately delay cancer progression. Consequently, we sought to investigate whether the two CAF types differentially affect cisplatin sensitivity and the underlying molecular mechanism. The secretion profile was examined by utilizing an antibody microarray with conditioned medium obtained from the co-culture of OSCC cells and two types of primary CAFs. The effect of CAF-dependent factors on cisplatin resistance was investigated by utilizing conditioned media (CM) and extracellular vesicle (EVs) derived from CAFs. The impacts of candidate genes were confirmed using gain- and loss-of-function analyses in spheroids and organoids, and a mouse xenograft. Lastly, we compared the expression pattern of the candidate genes in tissues from OSCC patients exhibiting different responses to cisplatin. When OSCC cells were cultured with conditioned media (CM) from the two different CAF groups, cisplatin resistance increased only under CAF-P CM. OSCC cells specifically expressed insulin-like growth factor binding protein 3 () after co-culture with CAF-D. Meanwhile, -knockdown OSCC cells acquired cisplatin resistance in CAF-D CM. expression was promoted by GATA-binding protein 1 (), a transcription factor targeted by miR-876-3p, which was enriched only in CAF-P-derived EV. Treatment with CAF-P EV carrying miR-876-3p antagomir decreased cisplatin resistance compared to control miRNA-carrying CAF-P EV. On comparing the staining intensity between cisplatin-sensitive and -insensitive tissues from OSCC patients, there was a positive correlation between and expression and cisplatin sensitivity in OSCC tissues from patients. These results provide insights for overcoming cisplatin resistance, especially concerning EVs within the tumor microenvironment. Furthermore, it is anticipated that the expression levels of and miR-876-3p, along with , could aid in the prediction of cisplatin resistance.
铂类化疗药物常用于治疗实体肿瘤,但药物耐药性常常限制其疗效。癌症相关成纤维细胞(CAF)衍生的细胞外囊泡(EV)携带各种 miRNA,与化疗耐药性有关。然而,CAF 调节口腔鳞状细胞癌(OSCC)顺铂耐药的分子机制尚不清楚。我们采用了两种不同的原发性 CAF 类型,它们对癌症进展有不同的影响:CAF-P,代表更具侵袭性的促进癌症的类别,CAF-D,其特征是性质适度延迟癌症进展。因此,我们试图研究这两种 CAF 类型是否会对顺铂敏感性产生不同的影响,以及潜在的分子机制。通过利用 OSCC 细胞与两种类型的原发性 CAF 共培养获得的条件培养基,利用抗体微阵列检测分泌谱。利用 CAF 依赖性因子的条件培养基(CM)和细胞外囊泡(EV)研究其对顺铂耐药性的影响。利用球体和类器官以及小鼠异种移植的基因增益和缺失功能分析,确认候选基因的影响。最后,我们比较了候选基因在对顺铂反应不同的 OSCC 患者组织中的表达模式。当 OSCC 细胞与来自两种不同 CAF 组的条件培养基(CM)共培养时,只有在 CAF-P CM 下,顺铂耐药性才会增加。OSCC 细胞在与 CAF-D 共培养后特异性表达胰岛素样生长因子结合蛋白 3 ()。同时,-敲低的 OSCC 细胞在 CAF-D CM 中获得顺铂耐药性。转录因子 GATA 结合蛋白 1 ()促进了的表达,该转录因子是 miR-876-3p 的靶点,仅在 CAF-P 衍生的 EV 中富集。与对照 miRNA 携带的 CAF-P EV 相比,用携带 miR-876-3p 拮抗剂的 CAF-P EV 处理降低了顺铂耐药性。比较顺铂敏感和耐药的 OSCC 患者组织之间的染色强度,在顺铂敏感的 OSCC 组织中,与 表达呈正相关。这些结果为克服顺铂耐药性提供了新的见解,特别是针对肿瘤微环境中的 EV。此外,预计和 miR-876-3p 的表达水平以及的表达水平可以帮助预测顺铂耐药性。
Zotero 插件
