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基因表达:蛋白质相互作用系统网络建模鉴定卵巢癌中与转化相关的分子和途径。

Gene expression: protein interaction systems network modeling identifies transformation-associated molecules and pathways in ovarian cancer.

机构信息

National Centre for Cell Science, NCCS Complex and Institute of Bioinformatics & Biotechnology, Pune University, Pune, India.

出版信息

Cancer Res. 2010 Jun 15;70(12):4809-19. doi: 10.1158/0008-5472.CAN-10-0447. Epub 2010 Jun 8.

DOI:10.1158/0008-5472.CAN-10-0447
PMID:20530682
Abstract

Multiple, dissimilar genetic defects in cancers of the same origin contribute to heterogeneity in tumor phenotypes and therapeutic responses of patients, yet the associated molecular mechanisms remain elusive. Here, we show at the systems level that serous ovarian carcinoma is marked by the activation of interconnected modules associated with a specific gene set that was derived from three independent tumor-specific gene expression data sets. Network prediction algorithms combined with preestablished protein interaction networks and known functionalities affirmed the importance of genes associated with ovarian cancer as predictive biomarkers, besides "discovering" novel ones purely on the basis of interconnectivity, whose precise involvement remains to be investigated. Copy number alterations and aberrant epigenetic regulation were identified and validated as significant influences on gene expression. More importantly, three functional modules centering on c-Myc activation, altered retinoblastoma signaling, and p53/cell cycle/DNA damage repair pathways have been identified for their involvement in transformation-associated events. Further studies will assign significance to and aid the design of a panel of specific markers predictive of individual- and tumor-specific pathways. In the parlance of this emerging field, such networks of gene-hub interactions may define personalized therapeutic decisions.

摘要

多种不同的遗传缺陷导致同一来源的癌症在肿瘤表型和患者治疗反应方面存在异质性,但相关的分子机制仍不清楚。在这里,我们从系统水平上表明,浆液性卵巢癌的特征是与特定基因集相关的相互关联的模块被激活,该基因集源自三个独立的肿瘤特异性基因表达数据集。网络预测算法结合已建立的蛋白质相互作用网络和已知功能,肯定了与卵巢癌相关的基因作为预测生物标志物的重要性,除了“发现”仅基于连通性的新型基因,其确切的参与仍有待研究。拷贝数改变和异常的表观遗传调控被确定并验证为对基因表达有重要影响。更重要的是,已经确定了三个以 c-Myc 激活、视网膜母细胞瘤信号改变以及 p53/细胞周期/DNA 损伤修复途径为中心的功能模块,因为它们参与了与转化相关的事件。进一步的研究将赋予意义,并有助于设计一组特定的标记物,以预测个体和肿瘤特异性途径。用这个新兴领域的术语来说,这种基因枢纽相互作用网络可能定义了个性化的治疗决策。

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