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Extraction and Prioritization of a Gene-Cancer-By-Survival Network Involved in Homeostasis of Intracellular Calcium Concentrations Using TCGA PANCAN Data

机译:提取和优先级Gene-Cancer-By-Survival网络参与体内平衡的细胞内钙使用浓度,TCGA PANCAN数据

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Regulation of intracellular calcium concentrations, [Ca++]i is important in maintaining the viability of normal as well as cancer cells and can be mediated by tumor microenvironment. Calcium release-activated calcium channel protein (ORAI) calcium channels on the plasma membrane (PM) become physically connected by stromal interaction molecules (STIMs) to the endoplasmic reticulum (ER), on which paralogous receptors of inositol phosphate and of ryanodine are also present along with ATP2A/SERCA (sarco/endoplasmic reticulum calcium ATPases) subunits (also known as PM-ER geneset). Proper expression of this functionally and physically interconnected geneset is essential for the maintenance of [Ca++]i, yet has not been interrogated as a whole for its role in cancer prognosis using multivariable Cox regression. In the present study, we examined whether the expression profile of the PM-ER geneset exhibited prognostic significance across different cancers found in The Cancer Genome Atlas (TCGA) by generating gene-cancer-by-survival networks, in which the nodes represented either genes or cancers and the edges, the logarithmically transformed hazard ratios for overall survival (OS). We then applied network clustering to identify the gene-cancer subnetworks with high connectivity, among which uveal melanoma (UVM) emerged exhibiting the highest degree of genes (k = 10). BAP1, a well-known [Ca++]i regulator and a tumor suppressor, was not found to be significant in predicting OS by PM-ER geneset for UVM, yet it was for several others, including mesothelioma (MESO). Moreover, the best subset of the PM-ER geneset obtained by lasso predicted OS in the TCGA UVM cohort with an area under the receiver operating characteristics (AUC) of 91.4%, comparable to or better than previous prognostic signatures in the literature. Our findings indicate that homeostasis of [Ca++]i is an essential determinant of prognosis in multiple cancers and particularly in UVM. The proposed gene-cancer-by-survival network approach can be extended with other gene sets as well as different survival types.
机译:调节细胞内钙的浓度,(Ca + +)我是重要的维护正常的可行性以及癌症细胞,可以由肿瘤微环境。钙通道蛋白(ORAI)钙通道在质膜(PM)成为身体通过基质相互作用分子连接(敌人)内质网(ER)磷酸肌醇,paralogous受体阿诺定也存在一起ATP2A / SERCA(石棺/内质网钙atp酶)的子单元(也称为PM-ER geneset)。适当的功能和表达物理互连geneset是至关重要的(Ca + +)的维护我,但是没有审讯在癌症作为一个整体的作用使用多变量Cox回归预测。目前的研究中,我们检验表达谱的PM-ER geneset展出在不同的癌症预后的意义癌症基因组图谱(TCGA)生成gene-cancer-by-survival网络其中节点代表基因或癌症和边缘,对数转换风险比率总体存活率(OS)。识别高的gene-cancer子网连接,其中葡萄膜黑色素瘤(UVM)展示了最高程度的基因(k= 10)。肿瘤抑制基因,发现并不明显在预测系统由PM-ER geneset UVM,然而它几个人,包括间皮瘤吗(内消旋)。geneset套索预测获得的操作系统TCGA UVM队列接收器下面积操作特征(AUC)为91.4%,比先前的预后相当或更好签名在文献中。表明体内平衡(Ca + +)我是一个在多个预后的基本决定因素癌症和特别是UVM。gene-cancer-by-survival网络的方法与其他基因集以及扩展不同的生存类型。

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