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Profiling Bladder Cancer Organ Site-Specific Metastasis Identifies LAMC2 as a Novel Biomarker of Hematogenous Dissemination

机译:分析膀胱癌器官特定部位的转移可将LAMC2鉴定为血行播散的新型生物标志物

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摘要

Little is known about which genes mediate metastasis in bladder cancer, which accounts for much of the mortality of this disease. We used human bladder cancer cell lines to develop models of two clinically common metastatic sites, lung and liver, and evaluated their gene expression with respect to human tumor tissues. Parental cells were injected into either the murine spleen to generate liver metastases or tail vein to generate lung metastases with sequential progeny derived by re-injection and comparisons made of their organ-specific nature by crossed-site injections. Both genomic and transcriptomic analyses of organ-selected cell lines found salient differences and shared core metastatic profiles, which were then screened against gene expression data from human tumors. The expression levels of laminin V gamma 2 (LAMC2) contained in the core metastatic signature were increased as a function of human tumor stage, and its genomic location was in an area of gain as measured by comparative genomic hybridization. Using immunohistochemistry in a human bladder cancer tissue microarray, LAMC2 expression levels were associated with tumor grade, but inversely with nodal status. In contrast, in node-negative patients, LAMC2 expression was associated with visceral metastatic recurrence. In summary, LAMC2 is a novel biomarker of bladder cancer metastasis that reflects the propensity of cells to metastasize via either lymphatic or hematogenous routes.
机译:对于哪些基因介导膀胱癌的转移知之甚少,这占该疾病死亡率的大部分。我们使用人膀胱癌细胞系开发了两个临床上常见的转移部位(肺和肝)的模型,并评估了它们相对于人肿瘤组织的基因表达。将亲本细胞注射到鼠脾中以产生肝转移瘤或尾静脉以产生肺转移瘤,其具有通过重新注射产生的连续后代,并通过交叉位点注射比较它们的器官特异性。器官选择细胞系的基因组和转录组分析都发现了显着差异和共有的核心转移谱,然后针对人类肿瘤的基因表达数据进行了筛选。核心转移标记中包含的层粘连蛋白Vγ2(LAMC2)的表达水平随人肿瘤阶段的增加而增加,并且其基因组位置位于通过比较基因组杂交测量的获得区域中。在人膀胱癌组织微阵列中使用免疫组化技术,LAMC2表达水平与肿瘤等级相关,但与淋巴结状态成反比。相反,在淋巴结阴性患者中,LAMC2表达与内脏转移复发有关。总之,LAMC2是膀胱癌转移的一种新型生物标志物,它反映了细胞通过淋巴或血源性途径转移的倾向。

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