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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Elevated expression of the centromere protein-A(CENP-A)-encoding gene as a prognostic and predictive biomarker in human cancers
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Elevated expression of the centromere protein-A(CENP-A)-encoding gene as a prognostic and predictive biomarker in human cancers

机译:着丝粒蛋白-A(CENP-A)编码基因的表达升高,作为人类癌症的预后和预测生物标志物

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Centromere protein-A (CENP-A), a histone-H3 variant, plays an essential role in cell division by ensuring proper formation and function of centromeres and kinetochores. Elevated CENP-A expression has been associated with cancer development. This study aimed to establish whether elevated CENP-A expression can be used as a prognostic and predictive cancer biomarker. Molecular profiling of CENP-A in human cancers was investigated using genomic, transcriptomic and patient information from databases, including COSMIC, Oncomine, Kaplan-Meier plotter and cBioPortal. A network of CENP-A co-expressed genes was derived from cBioPortal and analyzed using Ingenuity Pathway Analysis (IPA) and Oncomine protocols to explore the function of CENP-A and its predictive potential. Transcriptional and post-transcriptional regulation of CENP-A expression was analyzed in silico. It was found that CENP-A expression was elevated in 20 types of solid cancer compared with normal counterparts. Elevated CENP-A expression highly correlated with cancer progression and poor patient outcome. Genomic analysis indicated that the elevated CENP-A expression was not due to alterations in the sequence or copy number of the CENP-A gene. Furthermore, CENP-A can be regulated by key oncogenic proteins and tumor-suppressive microRNAs. CENP-A co-expression network analysis indicated that CENP-A function is associated with cell cycle progression. Oncomine analysis showed a strong correlation between elevated CENP-A expression and oncolytic response of breast cancer patients to taxane-based chemotherapy. In conclusion, elevated CENP-A expression is coupled to malignant progression of numerous types of cancer. It may be useful as a biomarker of poor patient prognosis and as a predictive biomarker for taxane-based chemotherapy.
机译:着丝粒蛋白A(CENP-A),一种组蛋白H3变体,通过确保着丝粒和动植物的正确形成和功能,在细胞分裂中起着至关重要的作用。 CENP-A表达升高与癌症的发展有关。这项研究旨在确定升高的CENP-A表达是否可以用作预后和预测性癌症生物标志物。使用来自COSMIC,Oncomine,Kaplan-Meier绘图仪和cBioPortal等数据库的基因组,转录组学和患者信息,研究了人类癌症中CENP-A的分子谱。 CENP-A共表达基因的网络是从cBioPortal衍生而来的,并使用了机能途径分析(IPA)和Oncomine协议进行了分析,以探索CENP-A的功能及其预测潜力。在计算机上分析了CENP-A表达的转录和转录后调控。发现与正常对应物相比,在20种实体癌中CENP-A表达升高。 CENP-A表达升高与癌症进展和不良患者预后高度相关。基因组分析表明,CENP-A表达的升高并非归因于CENP-A基因序列或拷贝数的改变。此外,CENP-A可以由关键的致癌蛋白和抑制肿瘤的microRNA调控。 CENP-A共表达网络分析表明,CENP-A功能与细胞周期进程有关。 Oncomine分析显示乳腺癌患者对紫杉烷类化学疗法的CENP-A表达升高与溶瘤反应密切相关。总之,CENP-A表达升高与多种类型的癌症的恶性进展相关。它可以用作患者预后不良的生物标志物,也可以用作基于紫杉烷类化学疗法的预测性生物标志物。

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