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Evolution of unbalanced gain of distal chromosome 2p in neuroblastoma

机译:神经母细胞瘤远端染色体2p失衡增益的演变

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摘要

Neuroblastoma, one of the most common tumors of childhood, presents at diagnosis with a vast number of recurrent chromosomal imbalances that include hyperdiploidy for whole chromosomes, partial loss of 1p, 3p, 4p, 11q, 14q, partial gain of 1q, 7q, 17q and amplification of MYCN. These abnormalities are nonrandomly distributed in neuroblastoma as loss of 3p and 11q rarely occur in MYCN amplified neuroblastomas. Here, we report on a patient who had a non-MYCN amplified 3p-/11q- neuroblastoma at diagnosis who subsequently developed a high level of MYCN amplification in bone marrow metastases 41 months after induction of complete remission. The tumor at diagnosis had low level unbalanced gain of distal 2p. In order to assess the frequency of low level gain of distal 2p in neuroblastoma, we examined the comparative genomic hybridization results from 60 neuroblastomas. Among non-MYCN amplified neuroblastomas, 8/45 (18%) had low level gain of distal 2p. Low level gain for a segment of 2p (i.e. a region larger than the 2p23→p24 undergoing amplification) was also detected in five of the 15 tumors that had high level MYCN amplification. The possibility that low level gain of distal 2p is a risk factor for high level MYCN amplification is discussed.
机译:神经母细胞瘤是儿童最常见的肿瘤之一,在诊断时表现为大量复发性染色体失衡,包括整个染色体的超二倍体性,部分丢失1p,3p,4p,11q,14q,部分丢失1q,7q,17q和扩增MYCN。这些异常在神经母细胞瘤中是非随机分布的,因为在MYCN扩增的神经母细胞瘤中很少发生3p和11q的丢失。在这里,我们报道了一名在诊断中患有非MYCN扩增的3p- / 11q-神经母细胞瘤的患者,该患者随后在诱导完全缓解后41个月的骨髓转移中发展了高水平的MYCN扩增。诊断时的肿瘤远端2p的水平不平衡增益较低。为了评估神经母细胞瘤远端2p低水平增益的频率,我们检查了来自60个神经母细胞瘤的比较基因组杂交结果。在非MYCN扩增的神经母细胞瘤中,8/45(18%)的远端2p水平增高。在15个具有高水平MYCN扩增的肿瘤中,有5个也检测到2p片段(即大于2p23→p24的区域)的低水平增益。讨论了远端2p的低水平增益是MYCN高水平扩增的危险因素的可能性。

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