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Array painting reveals a high frequency of balanced translocations in breast cancer cell lines that break in cancer-relevant genes

机译:阵列绘画揭示了患有癌症相关基因的乳腺癌细胞系中的高频率平衡易位性

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Chromosome translocations in the common epithelial cancers are abundant, yet little is known about them. They have been thought to be almost all unbalanced and therefore dismissed as mostly mediating tumour suppressor loss. We present a comprehensive analysis by array painting of the chromosome translocations of breast cancer cell lines HCC1806, HCC1187 and ZR-75-30. In array painting, chromosomes are isolated by flow cytometry, amplified and hybridized to DNA microarrays. A total of 200 breakpoints were identified and all were mapped to 1?Mb resolution on bacterial artificial chromosome (BAC) arrays, then 40 selected breakpoints, including all balanced breakpoints, were further mapped on tiling-path BAC arrays or to around 2?kb resolution using oligonucleotide arrays. Many more of the translocations were balanced at 1?Mb resolution than expected, either reciprocal (eight in total) or balanced for at least one participating chromosome (19 paired breakpoints). Second, many of the breakpoints were at genes that are plausible targets of oncogenic translocation, including balanced breaks at CTCF, EP300/p300 and FOXP4. Two gene fusions were demonstrated, TAX1BP1–AHCY and RIF1–PKD1L1. Our results support the idea that chromosome rearrangements may play an important role in common epithelial cancers such as breast cancer.
机译:常见上皮癌中的染色体易位是丰富的,但对它们而言很少。他们被认为几乎所有人都不平衡,因此被视为大多介导肿瘤抑制损失。我们通过阵列绘制乳腺癌细胞系HCC1806,HCC1187和ZR-75-30阵列绘画综合分析。在阵列涂装中,通过流式细胞术分离染色体,扩增并与DNA微阵列杂交。鉴定了200个断点,均被映射到1?MB分辨率对细菌人工染色体(BAC)阵列,然后将40个选定断裂点(包括所有平衡断点)进一步映射到百帘球阵列或大约2?KB使用寡核苷酸阵列分辨率。许多易位性均衡为1?MB分辨率比预期的分辨率相当,互易(总共八个)或至少一个参与染色体(19个成对断点)平衡。其次,许多断点是在致癌易位的合理靶向的基因中,包括CTCF,EP300 / P300和FOXP4的平衡破裂。证明了两种基因融合,税1BP1-Ahcy和RIF1-PKD1L1。我们的研究结果支持染色体重排可能在诸如乳腺癌等常见上皮癌中发挥重要作用。

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