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ITGA3 and ITGB4 expression biomarkers estimate the risks of locoregional and hematogenous dissemination of oral squamous cell carcinoma

机译:ITGA3和ITGB4表达生物标志物评估口腔鳞状细胞癌局部扩散和血源性传播的风险

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Background Molecular biomarkers are essential for monitoring treatment effects, predicting prognosis, and improving survival rate in oral squamous cell carcinoma. This study sought to verify the effectiveness of two integrin gene expression ratios as biomarkers. Methods Gene expression analyses of integrin α3 (ITGA3), integrin β4 ( ITGB4 ), CD9 antigen ( CD9 ), and plakoglobin ( JUP ) by quantitative real-time PCR were conducted on total RNA from 270 OSCC cases. The logrank test, Cox proportional hazards model, and Kaplan-Meier estimates were performed on the gene expression ratios of ITGA3/CD9 and ITGB4/JUP and on the clinicopathological parameters for major clinical events. Results A high rate (around 80%) of lymph node metastasis was found in cases with a high ITGA3/CD9 ratio (high-ITGA3/CD9) and invasive histopathology (YK4). Primary site recurrence (PSR) was associated with high-ITGA3/CD9, T3-4 (TNM class), and positive margin, indicating that PSR is synergistically influenced by treatment failure and biological malignancy. A high ITGB4/JUP ratio (high-ITGB4/JUP) was revealed to be a primary contributor to distant metastasis without the involvement of clinicopathological factors, suggesting intervention of a critical step dependent on the function of the integrin β4 subunit. Kaplan-Meier curves revealed positive margin as a lethal treatment consequence in high-ITGA3/CD9 and YK4 double-positive cases. Conclusion Two types of metastatic trait were found in OSCC: locoregional dissemination, which was reflected by high-ITGA3/CD9, and distant metastasis through hematogenous dissemination, uniquely distinguished by high-ITGB4/JUP. The clinical significance of the integrin biomarkers implies that biological mechanisms such as cancer cell motility and anchorage-independent survival are vital for OSCC recurrence and metastasis.
机译:背景技术分子生物标志物对于监测口腔鳞状细胞癌的治疗效果,预测预后和提高生存率至关重要。这项研究试图验证两种整合素基因表达比例作为生物标志物的有效性。方法采用定量实时荧光定量PCR技术对270例OSCC患者的总RNA进行整合素α3(ITGA3),整合素β4(ITGB4),CD9抗原(CD9)和斑白蛋白(JUP)的基因表达分析。对ITGA3 / CD9和ITGB4 / JUP的基因表达比例以及主要临床事件的临床病理参数进行了logrank检验,Cox比例风险模型和Kaplan-Meier估计。结果在高ITGA3 / CD9比(高ITGA3 / CD9)和浸润性组织病理学(YK4)的病例中,淋巴结转移率很高(约80%)。原发部位复发(PSR)与高ITGA3 / CD9,T3-4(TNM类)和阳性切缘相关,表明PSR受到治疗失败和生物恶性的协同影响。高ITGB4 / JUP比(high-ITGB4 / JUP)被认为是远处转移的主要诱因,而没有临床病理因素的参与,提示关键步骤的干预取决于整联蛋白β4亚基的功能。 Kaplan-Meier曲线显示在高ITGA3 / CD9和YK4双阳性病例中,作为致命治疗结果的阳性切缘。结论在OSCC中发现了两种类型的转移性状:局部区域性播散,其通过高ITGA3 / CD9反映出来;和远距离转移通过血源性播散,其独特之处在于高ITGB4 / JUP。整联蛋白生物标志物的临床意义表明,诸如癌细胞运动性和不依赖锚固的存活等生物学机制对于OSCC复发和转移至关重要。

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