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多项基因表达研究中发现的卵巢癌新潜在配体-受体信号传导环。

New potential ligand-receptor signaling loops in ovarian cancer identified in multiple gene expression studies.

作者信息

Castellano Giancarlo, Reid James F, Alberti Paola, Carcangiu Maria Luisa, Tomassetti Antonella, Canevari Silvana

机构信息

Unit of Molecular Therapies, Department of Experimental Oncology, Istituto Nazionale Tumori FIRC di Oncologia Molecolare, Milan, Italy.

出版信息

Cancer Res. 2006 Nov 15;66(22):10709-19. doi: 10.1158/0008-5472.CAN-06-1327. Epub 2006 Nov 6.

DOI:10.1158/0008-5472.CAN-06-1327
PMID:17090524
Abstract

Based on the hypothesis that gene products involved in the same biological process would be coupled at transcriptional level, a previous study analyzed the correlation of the gene expression patterns of ligand-receptor (L-R) pairs to discover potential autocrine/paracrine signaling loops in different cancers (Graeber and Eisenberg. Nat Genet 2001; 29:295). By refining the starting database, a list of 511 L-R pairs was compiled, combined to eight data sets from a single pathology, epithelial ovarian cancer, and examined as a proof-of-principle of the statistical and biological validity of the correlation of the L-R gene expression patterns in cancer. Analysis revealed a Bonferroni-corrected significant correlation of 105 L-R pairs in at least one data set and, by systematic analysis, identified 39 more frequently correlated L-R pairs, 7 of which were already biologically confirmed. In four data sets examined for an L-R correlation associated with patient survival time, 15 L-R pairs were significantly correlated in short surviving patients in two of the data sets. Immunohistochemical analysis of one of the newly identified correlated L-R pairs (i.e., EFNB3-EPHB4) revealed the correlated expression of ephrin-B3 and EphB4 proteins in 45 of 55 epithelial ovarian tumor samples (P < 0.0001). Together, these data not only support the validity of cross-comparison analysis of gene expression data because known and expected correlations were confirmed but also point to the promise of such analysis in identifying new L-R signaling loops in cancer.

摘要

基于参与相同生物学过程的基因产物在转录水平上会相互关联这一假设,先前的一项研究分析了配体 - 受体(L - R)对的基因表达模式之间的相关性,以发现不同癌症中潜在的自分泌/旁分泌信号环(格雷伯和艾森伯格。《自然遗传学》2001年;29:295)。通过完善起始数据库,编制了一份包含511个L - R对的列表,并将其与来自单一病理类型——上皮性卵巢癌的八个数据集相结合,作为癌症中L - R基因表达模式相关性的统计和生物学有效性的原理验证进行研究。分析显示,在至少一个数据集中,105个L - R对经邦费罗尼校正后具有显著相关性,并且通过系统分析,又确定了39个更常出现相关性的L - R对,其中7个已得到生物学证实。在针对与患者生存时间相关的L - R相关性进行检测的四个数据集中,有两个数据集显示,在短期存活患者中,15个L - R对具有显著相关性。对新确定的一对相关L - R(即EFNB3 - EPHB4)进行免疫组织化学分析发现,在55个上皮性卵巢肿瘤样本中的45个样本中,ephrin - B3和EphB4蛋白呈相关表达(P < 0.0001)。总之,这些数据不仅支持了基因表达数据交叉比较分析的有效性,因为已知和预期的相关性得到了证实,而且还指出了这种分析在识别癌症中新的L - R信号环方面的前景。

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