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Comprehensive analysis on the expression levels and prognostic values of LOX family genes in kidney renal clear cell carcinoma

机译:肾肾透明细胞癌LOX家族基因表达水平及预后价综合分析

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Backgrounds Kidney renal clear cell carcinoma (KIRC) is a major pathological type of renal cell carcinoma (RCC), and the prognosis of advanced KIRC patients is often unsatisfactory. Some lysine oxidase (LOX) family genes have been proven to be upregulated in some malignancies and play pivotal roles in the carcinogenesis. However, their roles in KIRC remain unclear. Materials and Methods Here, we used some online databases (eg, ONCOMINE, GEPIA, UALCAN, c‐BioPortal, Human Protein Altas) to comprehensively explored the expression levels and the prognostic values of LOX family genes in KIRC using bioinformatic methods. Results The results revealed that lysyl oxidase (LOX) and lysyl oxidase‐like 2 (LOXL2) were significantly overexpressed in KIRC at the level of mRNA expression, protein expression, and RCC cell lines. Further analysis demonstrated that higher mRNA expression of LOX and LOXL2 were significantly correlated with poor survival, tumor grade, individual cancer stages, and nodal metastasis status. DNA copy number amplifications and mRNA upregulation, DNA deep deletion, and mRNA upregulation were the main genetic mutations of LOX and LOXL2, respectively. Prognostic analysis showed that the altered group had significantly poorer overall survival (OS) compared to the unaltered group (p?=?.0387). Co‐expression analysis showed CP, PLOD2, and COL5A1 were significantly correlated with LOX, and COL1A2 was positively correlated with LOXL2. Further analysis confirmed that these co‐expressed genes were significantly upregulated and predicted unfavorable prognosis in KIRC. Conclusion Multi‐level analysis demonstrated that LOX and LOXL2 were significantly upregulated and predicted poor survival in KIRC, which may apply as promising biomarkers for diagnosis and therapy of KIRC in the future.
机译:背景技术肾脏肾透明细胞癌(KIRC)是一种主要的病理类型的肾细胞癌(RCC),先进的KIRC患者的预后往往不满意。已经证明一些赖氨酸氧化酶(LOX)家族基因在一些恶性肿瘤中上调并在致癌物中发挥枢转作用。然而,他们在kirc中的角色仍然不清楚。这里的材料和方法,我们使用了一些在线数据库(例如,oncomsine,Gepia,uAlcan,C-Bioportal,人蛋白ALTA),通过生物信息方法综合探索kirc中Lox家族基因的表达水平和预后值。结果结果表明,在mRNA表达,蛋白表达和RCC细胞系的水平下,赖氨酸氧化酶(LOX)和赖氨酸氧化酶样2(LOXL2)在KIRC中显着过表达。进一步的分析表明,LOX和LOX12的较高mRNA表达与差的存活,肿瘤级,个体癌症阶段和节点转移状态显着相关。 DNA拷贝数扩增和mRNA上调,DNA深缺失和mRNA上调分别是LOX和LOX12的主要基因突变。预后分析表明,与未改变的组相比,改变的组在整体存活率(OS)显着较差(P?= 0387)。共表达分析显示CP,PLOD2和COL5A1与LOX显着相关,COL1A2与LOXL2呈正相关。进一步的分析证实,这些共表达基因显着上调并预测了KIRC的不利预后。结论多级分析表明,LOX和LOX12显着上调并预测kirc存活率可差,这可能是未来脊髓克尔诊断和治疗的有前途的生物标志物。

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