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Coexpression of SFRP1 and WIF1 as a Prognostic Predictor of Favorable Outcomes in Patients with Colorectal Carcinoma

机译:SFRP1和WIF1的共表达作为结直肠癌患者预后良好的预后指标

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摘要

Colorectal tumorigenesis is ascribed to the activity of Wnt signaling pathway in a ligand-independent manner mainly through APC and CTNNB1 gene mutations and in a ligand-dependent manner through low expression of Wnt inhibitors such as WNT inhibitory factor 1 (WIF1) and secreted frizzled related protein 1 (SFRP1). In this study we found that WIF1 protein expression was increased and SFRP1 was decreased significantly in CRC tissue versus normal tissue, and high expression of WIF1 was associated with big tumor diameters and deep invasion, and loss of SFRP1 expression was associated with the left lesion site, deep invasion, and high TNM stage. Among the four expression patterns (WIF+/SFRP1+, WIF+/SFRP1-, WIF-/SFRP1+, and WIF-/SFRP1-) only coexpression of WIF1 and SFRP1 (WIF+/SFRP1+) was associated with favorable overall survival, together with low TNM stage, as an independent prognostic factor as shown in a multivariate survival model. The results indicated that WIF1 seemed to play an oncogenic role, while SFRP1 seemed to play an oncosuppressive role although both of them are secreted Wnt antagonists. Coexpression of SFRP1 and WIF1, rather than SFRP1 or WIF1 alone, could be used, together with low TNM stage, as a prognostic predictor of favorable outcomes in CRC.
机译:大肠癌的发生归因于Wnt信号通路的活性,主要通过APC和CTNNB1基因突变以配体非依赖性方式发生,而通过Wnt抑制剂(如WNT抑制因子1(WIF1))的低表达与配体依赖性方式则与分泌性卷曲相关蛋白1(SFRP1)。在这项研究中,我们发现CRC组织中的WIF1蛋白表达增加而SFRP1显着降低,而正常组织中WIF1的高表达与大肿瘤直径和深部浸润有关,而SFRP1表达的丧失与左病变部位有关,深度入侵和高TNM阶段。在四种表达模式(WIF + / SFRP1 +,WIF + / SFRP1-,WIF- / SFRP1 +和WIF- / SFRP1-)中,仅WIF1和SFRP1(WIF + / SFRP1 +)的共表达与总体生存期良好以及TNM分期低有关,作为多因素生存模型中显示的独立预后因素。结果表明,WIF1似乎起着致癌作用,而SFRP1似乎起着抑癌作用,尽管它们都是分泌的Wnt拮抗剂。 SFRP1和WIF1的共表达,而不是单独的SFRP1或WIF1,可与低TNM分期一起使用,作为预后良好的CRC预测指标。

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