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Contextualizing the Genes Altered in Bladder Neoplasms in Pediatric andTeen Patients Allows Identifying Two Main Classes of Biological ProcessesInvolved and New Potential Therapeutic Targets

机译:儿科和青少年患者膀胱肿瘤中改变的基因的背景信息化可以确定涉及的生物过程的两个主要类别和新的潜在治疗靶点

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摘要

Research on bladder neoplasms in pediatric and teen patients (BNPTP) has described 21 genes, which are variously involved in this disease and are mostly responsible for deregulated cell proliferation. However, due to the limited number of publications on this subject, it is still unclear what type of relationships there are among these genes and which are the chances that, while having different molecular functions, they i) act as downstream effector genes of well-known pro- or anti- proliferative stimuli and/or interplay with biochemical pathways having oncological relevance or ii) are specific and, possibly, early biomarkers of these pathologies. A Gene Ontology (GO)-based analysis showed that these 21 genes are involved in biological processes, which can be split into two main classes: cell regulation-based and differentiation/development-based. In order to understand the involvement/overlapping with main cancer-related pathways, we performed a meta-analysis dependent on the 189 oncogenic signatures of the Molecular Signatures Database (OSMSD) curated by the Broad Institute. We generated a binary matrix with 53 gene signatures having at least one hit; this analysis i) suggests that some genes of the original list show inconsistencies and might need to be experimentally re- assessed or evaluated as biomarkers (in particular, ACTA2) and ii) allows hypothesizing that important (proto)oncogenes (E2F3, ERBB2/HER2, CCND1, WNT1, and YAP1) and (putative) tumor suppressors (BRCA1, RBBP8/CTIP, and RB1-RBL2/p130) may participate in the onset of this disease or worsen the observed phenotype, thus expanding the list of possible molecular targets for the treatment of BNPTP.
机译:对儿童和青少年患者的膀胱肿瘤(BNPTP)的研究已经描述了21个基因,这些基因与该疾病有多种关系,并且主要负责细胞增殖失调。但是,由于有关该主题的出版物数量有限,目前尚不清楚这些基因之间存在何种类型的关系,以及尽管它们具有不同的分子功能,但它们有机会成为健康基因的下游效应基因。已知的促增殖或抗增殖刺激和/或与具有肿瘤学相关性的生化途径或ii)的相互作用是这些病理学的特异性且可能是早期生物标志物。基于基因本体论(GO)的分析表明,这21个基因参与了生物过程,可分为两大类:基于细胞调节和基于分化/发育。为了了解主要癌症相关途径的参与/重叠,我们进行了荟萃分析,该分析依赖于由Broad Institute策划的分子签名数据库(OSMSD)的189种致癌签名。我们生成了具有53个基因特征码的二进制矩阵,该基因特征码至少有一个命中点;该分析i)提示原始列表中的某些基因显示出不一致,可能需要通过实验重新评估或评估生物标记物(特别是ACTA2),并且ii)可以假设重要的(原)癌基因(E2F3,ERBB2 / HER2) ,CCND1,WNT1和YAP1)和(公认的)抑癌药(BRCA1,RBBP8 / CTIP和RB1-RBL2 / p130)可能参与该疾病的发作或使观察到的表型恶化,从而扩大了可能的分子靶点清单用于治疗BNPTP。

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