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Pancreatic Cancer Metastases Harbor Evidence of Polyclonality

机译:胰腺癌转移港口多克隆证据

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Studies of the cancer genome have demonstrated that tumors are composed of multiple subclones with varied genetic and phenotypic properties. However, little is known about how metastases arise and evolve from these subclones. To understand the cellular dynamics that drive metastasis, we used multicolor lineage-tracing technology in an autochthonous mouse model of pancreatic cancer. Here, we report that precursor lesions exhibit significant clonal heterogeneity but that this diversity decreases during premalignant progression. Furthermore, we present evidence that a significant fraction of metastases are polyclonally seeded by distinct tumor subclones. Finally, we show that clonality during metastatic growth-leading to either monoclonal or polyclonal expansion-differs based on the site of metastatic invasion. These results provide an unprecedented window into the cellular dynamics of tumor evolution and suggest that heterotypic interactions between tumor subpopulations contribute to metastatic progression in native tumors.
机译:癌症基因组的研究表明,肿瘤由具有不同遗传和表型特性的多个亚克隆组成。然而,关于这些亚克隆如何发生转移以及如何转移的了解甚少。为了了解驱动转移的细胞动力学,我们在胰腺癌的本地小鼠模型中使用了多色谱系追踪技术。在这里,我们报道,前体病变表现出明显的克隆异质性,但这种多样性在恶变前的进展过程中减少。此外,我们目前的证据表明,很大一部分转移灶是由不同的肿瘤亚克隆多克隆接种的。最后,我们显示了在转移生长过程中的克隆性会导致基于转移侵袭位点的单克隆或多克隆扩增差异。这些结果为了解肿瘤进化的细胞动力学提供了前所未有的窗口,并表明肿瘤亚群之间的异型相互作用有助于天然肿瘤的转移进程。

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