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Serine/threonine kinase 32C is overexpressed in bladder cancer and contributes to tumor progression

机译:丝氨酸/苏氨酸激酶32C在膀胱癌中过表达,有助于肿瘤进展

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摘要

Tumor markers of bladder cancer (BC) have been investigated for many years, but the clinical treatment based on these biomarkers is still unsatisfactory. STK32C, a member of the serine/threonine protein kinase of AGC superfamily, was first found to be highly expressed in brain tissues; however, the role of STK32C in malignant disease has not been determined. Data from TCGA database showed that the STK32C gene is overexpressed in BC and a number of other human tumors. In the current study, immunohistochemistry revealed that high expression of STK32C protein in tumor tissues was significantly associated with poor clinico pathologic features and a short relapse-free survival (RFS) in patients with BC. Slicing of STK32C inhibited tumor cell proliferation, migration and invasion in vitro. In vivo animal experiments demonstrated that knocking-down of STK32C restricted the growth of tumor cells in mice. Finally, microarray analysis revealed that silencing of STK32C inhibited the activity of the HMGB1 pathway and regulated the expression of key genes in this pathway. In conclusion, our study showed novel promoting roles for STK32C in human tumors, which may provide a new therapeutic target for the patients with BC.
机译:膀胱癌(BC)的肿瘤标志物已被研究多年,但基于这些生物标志物的临床治疗仍然不令人满意。 STK32C是AGC超家族的丝氨酸/苏氨酸蛋白激酶的成员,首先发现在脑组织中高度表达;然而,STK32C在恶性疾病中的作用尚未确定。来自TCGA数据库的数据显示STK32C基因在BC和许多其他人类肿瘤中过表达。在目前的研究中,免疫组织化学表明,肿瘤组织中STK32C蛋白的高表达与BC患者患者的临床病理特征和短期复发存活(RFS)显着相关。 STK32C的切片抑制肿瘤细胞增殖,体外迁移和侵袭。体内动物实验表明,STK32C的爆震限制了小鼠中肿瘤细胞的生长。最后,微阵列分析表明,STK32C的沉默抑制了HMGB1途径的活性,并调节了该途径中关键基因的表达。总之,我们的研究表明,人类肿瘤中STK32C的新型促进作用,这可能为BC患者提供新的治疗靶标。

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