Hassan Amani, Kungyal Tenzin, Zhou Shufeng, Blati Meryem, Finnson Kenneth, Bertos Nick, Golabi Nahid, Sadeghi Nader, Loganathan Sampath, Philip Anie
Divisions of Plastic Surgery, and Surgical and Interventional Sciences, Department of Surgery, McGill University, Montreal, QC, Canada.
Divisions of Thoracic and Upper GI Surgery, Department of Surgery, McGill University, Montreal, QC, Canada.
Exp Hematol Oncol. 2025 May 2;14(1):64. doi: 10.1186/s40164-025-00630-x.
Squamous cell carcinoma (SCC) is a prevalent malignancy and there are limited options to block the recurrence and metastasis that often occur in SCC patients. Although IL-6, a proinflammatory cytokine, is strongly implicated in SCC pathogenesis, its mechanism of action is poorly understood. The GPI-anchored membrane protein CD109 is frequently overexpressed in SCC and is associated with malignant transformation. The current study aims to investigate whether CD109 interacts with IL-6 receptor alpha (IL6Rα) and promotes IL-6-mediated oncogenic signaling to drive SCC progression.
IL6Rα interaction with CD109 was determined by coimmunoprecipitation, immunohistochemistry, immunofluorescence and FACS analysis using human SCC (oral and vulvar) cell lines and human oral SCC tumors versus control tissue. Regulation of IL-6-induced signaling and antioxidant responses by CD109 was analyzed via STAT3/NRF2/SOD1/HO1 pathway activation. Regulation of IL-6-mediated tumorigenicity by CD109 was determined using stem cell marker expression and a spheroid formation assay. Clinical validation was achieved using genomic and proteomic analysis of oral SCC tumors and of head and neck SCC patient data.
We show that CD109 interacts with and stabilizes IL6Rα expression and promotes IL-6/STAT3/NRF2 pathway in oral and vulvar SCC cells. Loss of CD109 attenuates this pathway leading to loss of cancer cell stemness and decreased expression of superoxide dismutase1 and heme oxygenase-1, antioxidant proteins important for cell survival after chemotherapy. Furthermore, clinical validation of these findings was achieved through multi-omic analysis of oral SCC tumors and of head and neck SCC patient data.
This work uncovers a previously unidentified mechanism in which CD109 serves as an essential regulator of IL6Rα expression and IL-6 mediated signaling in SCC cells, promoting stemness and antioxidant state, mechanisms known to mediate therapy resistance in SCC. Our findings establish a mechanistic validation for investigating the therapeutic utility of the CD109/ IL6Rα/STAT3/NRF2 pathway in SCC.
鳞状细胞癌(SCC)是一种常见的恶性肿瘤,对于阻断SCC患者中经常发生的复发和转移,可用的选择有限。尽管促炎细胞因子白细胞介素-6(IL-6)与SCC的发病机制密切相关,但其作用机制尚不清楚。糖基磷脂酰肌醇(GPI)锚定膜蛋白CD109在SCC中经常过度表达,并与恶性转化有关。本研究旨在探讨CD109是否与白细胞介素-6受体α(IL6Rα)相互作用,并促进IL-6介导的致癌信号传导以驱动SCC进展。
使用人SCC(口腔和外阴)细胞系、人口腔SCC肿瘤与对照组织,通过免疫共沉淀、免疫组织化学、免疫荧光和流式细胞术分析确定IL6Rα与CD109的相互作用。通过STAT3/NRF2/SOD1/HO1途径激活分析CD109对IL-6诱导的信号传导和抗氧化反应的调节。使用干细胞标志物表达和球状体形成试验确定CD109对IL-6介导的致瘤性的调节。通过对口腔SCC肿瘤和头颈部SCC患者数据的基因组和蛋白质组分析实现临床验证。
我们发现CD109与IL6Rα相互作用并稳定其表达,并促进口腔和外阴SCC细胞中的IL-6/STAT3/NRF2途径。CD109的缺失减弱了该途径,导致癌细胞干性丧失以及超氧化物歧化酶1和血红素加氧酶-1(对化疗后细胞存活很重要的抗氧化蛋白)的表达降低。此外,通过对口腔SCC肿瘤和头颈部SCC患者数据的多组学分析实现了这些发现的临床验证。
这项工作揭示了一种以前未被发现的机制,其中CD109作为SCC细胞中IL6Rα表达和IL-6介导的信号传导的重要调节因子,促进干性和抗氧化状态,这些机制已知介导SCC中的治疗抗性。我们的发现为研究CD109/IL6Rα/STAT3/NRF2途径在SCC中的治疗效用建立了机制验证。
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