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首页> 外文期刊>Brain pathology >Genome wide copy number abnormalities in pediatric medulloblastomas as assessed by array comparative genome hybridization.
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Genome wide copy number abnormalities in pediatric medulloblastomas as assessed by array comparative genome hybridization.

机译:通过阵列比较基因组杂交评估的小儿髓母细胞瘤中的基因组宽拷贝数异常。

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摘要

Array-based comparative genomic hybridization was used to characterize 22 medulloblastomas in order to precisely define genetic alterations in these malignant childhood brain tumors. The 17p(-)/17q(+) copy number abnormality (CNA), consistent with the formation of isochromosome 17q, was the most common event (8/22). Amplifications in this series included MYCL, MYCN and MYC previously implicated in medulloblastoma pathogenesis, as well as novel amplicons on chromosomes 2, 4, 11 and 12. Losses involving chromosomes 1, 2, 8, 10, 11, 16 and 19 and gains of chromosomes 4, 7, 8, 9 and 18 were seen in greater than 20% of tumors in this series. A homozygous deletion in 11p15 defines the minimal region of loss on this chromosome arm. In order to map the minimal regions involved in losses, gains and amplifications, we combined aCGH data from this series with that of two others obtained using the same RPCI BAC arrays. As a result of this combined analysis of 72 samples, we have defined specific regions on chromosomes 1, 8p, 10q, 11p and 16q which are frequently involved in CNAs in medulloblastomas. Using high density oligonucleotide expression arrays, candidate genes were identified within these consistently involved regions in a subset of the tumors.
机译:基于阵列的比较基因组杂交技术用于表征22个髓母细胞瘤,以精确定义这些恶性的儿童期脑肿瘤的遗传改变。最常见的事件是17p(-)/ 17q(+)拷贝数异常(CNA),与异染色体17q的形成一致。该系列的扩增包括先前与髓母细胞瘤发病有关的MYCL,MYCN和MYC,以及2、4、11和12号染色体上的新型扩增子。涉及1、2、8、10、11、16和19号染色体的损失以及在该系列中超过20%的肿瘤中可见4、7、8、9和18号染色体。 11p15中的纯合缺失定义了该染色体臂上的最小损失区域。为了绘制涉及损耗,增益和放大的最小区域,我们将来自该系列的aCGH数据与使用相同RPCI BAC阵列获得的其他两个数据相结合。通过对72个样本进行综合分析的结果,我们在染色体1、8p,10q,11p和16q上定义了特定区域,这些区域经常参与髓母细胞瘤中的CNA。使用高密度寡核苷酸表达阵列,在肿瘤子集的这些持续参与的区域内鉴定了候选基因。

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