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First Molecular Cytogenetic High Resolution Characterization of the NIH 3T3 Cell Line by Murine Multicolor Banding

机译:NIH 3T3细胞株通过小鼠多色条带的第一个分子细胞遗传学高分辨率表征。

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摘要

Since being established in 1963, the murine fibroblast cell line NIH 3T3 has been used in thousands of studies. NIH 3T3 immortalized spontaneously and became tetraploid shortly after its establishment. Here we report the first molecular cytogenetic characterization of NIH 3T3 using fluorescence in situ hybridization based multicolor banding (mcb). Overall, a complex rearranged karyotype presenting 16 breakpoints was characterized. Also it was possible to deduce the resulting gains and losses of copy numbers in NIH 3T3. Overall, only 1.8% of the NIH 3T3 genome is disome, 26.2% tri-, 60% tetra-, 10.8% quinta-, and 1.2% hexasome. Strikingly, the cell line gained only 4 derivative chromosomes since its first cytogenetic description in 1989. An attempt to align the observed imbalances of the studied cell line with their homologous regions in humans gave the following surprising result: NIH 3T3 shows imbalances as typically seen in human solid cancers of ectodermal origin.
机译:自1963年建立以来,鼠成纤维细胞系NIH 3T3已用于数千项研究中。 NIH 3T3自发永生,并在其建立后不久变成四倍体。在这里,我们报告基于荧光原位杂交的多色条带(mcb)的NIH 3T3的第一个分子细胞遗传学表征。总体而言,表征了复杂的重排核型,呈现16个断点。同样有可能推论出NIH 3T3的拷贝数的得失。总体而言,NIH 3T3基因组中只有1.8%是二基因组,三重基因组为26.2%,四重基因组为60%,五重奏基体为10.8%,六聚体为1.2%。令人惊讶的是,自1989年首次细胞遗传学描述以来,该细胞系仅获得了4条衍生染色体。试图将观察到的研究细胞系与人类同源区域的失衡进行比对,得出了以下令人惊讶的结果:NIH 3T3显示了失衡。外胚层来源的人类实体癌。

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