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Transmembrane protein 170B is a novel breast tumorigenesis suppressor gene that inhibits the Wnt/β-catenin pathway

机译:跨膜蛋白170B是抑制Wnt /β-catenin途径的新型乳腺肿瘤发生抑制基因

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The identification of specific drug targets guides the development of precise cancer treatments. Compared with oncogenes, tumor suppressor genes have been poorly studied in the treatment of breast cancer. We integrate the microRNA expression array from GEO (Gene Expression Omnibus) and TCGA (The Cancer Genome Atlas) databases in clinical breast cancer tissues, and find that miR-27a is significantly upregulated and correlated with poor survival outcome and tumor progression. Transmembrane protein 170B (TMEM170B), a new functional target of miR-27a, is identified via target prediction and experimental validation, suppressing breast cancer proliferation, metastasis, and tumorigenesis. Furthermore, TMEM170B overexpression promotes cytoplasmic β-catenin phosphorylation, resulting in the inhibition of β-catenin stabilization, reduction of nuclear β-catenin levels and downstream targets expression. Clinically, TMEM170B or β-catenin expression is significantly correlated with overall survival ratio in breast cancer patients. Thus, these results highlight TMEM170B as a novel tumor suppressor target in association with the β-catenin pathway, which may provide a new therapeutic approach for human breast cancer therapy.
机译:特定药物靶标的鉴定可指导精确癌症治疗的发展。与癌基因相比,在乳腺癌的治疗中对肿瘤抑制基因的研究很少。我们在临床乳腺癌组织中整合了来自GEO(基因表达综合)和TCGA(癌症基因组图谱)数据库的microRNA表达阵列,发现miR-27a显着上调并与不良的生存结果和肿瘤进展相关。跨膜蛋白170B(TMEM170B)是miR-27a的新功能靶标,可通过靶标预测和实验验证来鉴定,可抑制乳腺癌的增殖,转移和肿瘤发生。此外,TMEM170B过表达促进细胞质β-catenin磷酸化,从而抑制β-catenin稳定,降低核β-catenin水平和下游靶标表达。在临床上,TMEM170B或β-catenin的表达与乳腺癌患者的总生存率显着相关。因此,这些结果强调了TMEM170B是与β-catenin途径相关的新型肿瘤抑制靶标,这可能为人类乳腺癌治疗提供一种新的治疗方法。

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