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Stable Karyotypes in Epithelial Cancer Cell Lines Despite High Rates of Ongoing Structural and Numerical Chromosomal Instability

机译:尽管持续不断的结构和数值染色体不稳定性的发生率很高,但上皮癌细胞系中的核型却稳定

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摘要

Most human tumors and tumor cell lines exhibit numerical and structural chromosomal abnormalities. The goal of this study was to determine the ongoing rates of structural and numerical instability in selected cancer cell lines and to investigate the consequences of these rates to karyotypic progression. We studied two colorectal (HCT-116 and HT-29) and two ovarian (SKOV-3 and OVCAR-8) cancer cell lines and their single cell subclones. We found that the signature karyotypes of all four cell lines were distinct and each aberrant. Whereas high rates of ongoing structural and/or numerical chromosomal instability could be demonstrated in all cell lines, there was a relative stability of the consensus karyotype over many generations. No new clonal structural chromosomal reconfigurations emerged and the few numerical changes of karyotypes were restricted to abnormal chromosomes. This implies a kind of genomic optimization under the conditions of cell culture and suggests a link between genomic stabilization and cell propagation. We have been able to support this possibility by computer modeling. We did not observe a profound difference in the rates of numerical or structural instability in the cell lines with a replication error phenotype (RER+) versus the other cell lines.
机译:大多数人类肿瘤和肿瘤细胞系表现出数字和结构染色体异常。这项研究的目的是确定所选癌细胞系中结构和数字不稳定性的持续速率,并研究这些速率对核型进展的影响。我们研究了两个结直肠癌(HCT-116和HT-29)和两个卵巢癌(SKOV-3和OVCAR-8)癌细胞系及其单细胞亚克隆。我们发现所有四个细胞系的签名核型是不同的,每个异常。尽管在所有细胞系中都可以证明正在进行的结构和/或数字染色体不稳定性的发生率很高,但是共有核型在许多世代中都具有相对的稳定性。没有新的克隆结构染色体重组出现,并且核型的少数数值变化仅限于异常染色体。这意味着在细胞培养条件下的一种基因组优化,并暗示了基因组稳定与细胞繁殖之间的联系。我们已经能够通过计算机建模来支持这种可能性。我们没有观察到具有复制错误表型(RER +)的细胞系相对于其他细胞系的数字或结构不稳定性发生率的显着差异。

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