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TERT biology and function in cancer: beyond immortalisation

机译:TERT生物学和癌症功能:永生不朽

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Evasion of replicative senescence and proliferation without restriction, sometimes designated as immortalisation, is one of the hallmarks of cancer that may be attained through reactivation of telomerase in somatic cells. In contrast to most normal cells in which there is lack of telomerase activity, upregulation of TERT transcription/activity is detected in 80–90% of malignant tumours. In several types of cancer, there is a relationship between the presence of TERT promoter mutations, TERT mRNA expression and clinicopathological features, but the biological bridge between the occurrence of TERT promoter mutations and the aggressive/invasive features displayed by the tumours remains unidentified. We and others have associated the presence of TERT promoter mutations with metastisation/survival in several types of cancer. In follicular cell-derived thyroid cancer, such mutations are associated with worse prognostic features (age of patients, tumour size and tumour stage) as well as with distant metastases, worse response to treatment and poorer survival. In this review, we analyse the data reported in several studies that imply TERT transcription reactivation/activity with cell proliferation, tumour invasion and metastisation. A particular attention is given to the putative connections between TERT transcriptional reactivation and signalling pathways frequently altered in cancer, such as c-MYC, NF-κB and B-Catenin.
机译:不受限制地复制性衰老和增殖的逃避,有时被称为永生化,是通过在体细胞中激活端粒酶可以达到的癌症标志之一。与大多数缺乏端粒酶活性的正常细胞相比,在80–90%的恶性肿瘤中检测到TERT转录/活性的上调。在几种类型的癌症中,TERT启动子突变的存在,TERT mRNA表达与临床病理特征之间存在关联,但是,TERT启动子突变的发生与肿瘤所表现出的侵袭性/侵袭性特征之间的生物学桥梁仍然不确定。我们和其他人将TERT启动子突变的存在与几种类型的癌症的转移/生存相关联。在滤泡细胞源性甲状腺癌中,此类突变与预后较差(患者年龄,肿瘤大小和肿瘤分期)以及远处转移,对治疗的反应较差和生存期较差有关。在这篇综述中,我们分析了几项研究中报告的数据,这些数据暗示TERT转录再激活/具有细胞增殖,肿瘤侵袭和转移的活性。特别注意TERT转录激活与癌症中经常改变的信号通路之间的假定联系,例如c-MYC,NF-κB和B-连环素。

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