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首页> 外文期刊>British Journal of Cancer >An increased NM23H1 copy number may be a poor prognostic factor independent of LOH on 1p in neuroblastomas
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An increased NM23H1 copy number may be a poor prognostic factor independent of LOH on 1p in neuroblastomas

机译:NM23H1拷贝数增加可能是不良的预后因素,独立于神经母细胞瘤中1p的LOH

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In a study of 154 neuroblastomas, loss of heterozygosity (LOH) was observed on 1p (13%, 19/143), 11q (19%, 11/59), 14q (15%, 15/97), 17p (5%, 5/105) and 17q (17%, 9/52). We also found an increase in NM23H1 copy number in 14% (13/95) of neuroblastomas. All except one tumour with an increased copy number stained positive with anti-NM23H1 monoclonal antibody. Event-free survival (EFS) was significantly shorter in 19 patients with LOH on 1p than in 128 without (41% vs 77% 4 year EFS, P=0.0093), and in 13 patients with increased NM23H1 copy numbers than in 82 with normal copy numbers of the gene (61% vs 84% 4 year EFS, P=0.0103). LOH on 11q, 14q or 17q did not affect EFS. Most tumours with LOH on 1p, increased NM23H1 copy numbers or MYCN amplification occurred in patients aged 12 months or more, those with advanced stage disease, and those who showed near diploidy or pseudodiploidy. However, LOH on 1p was found in only 1 of the 13 tumours with increased NM23H1 copy numbers, and MYCN amplification of four copies occurred in only one other such tumour. These findings suggest that the increased NM23H1 copy number may be a predictor for poor prognosis, independent of LOH on 1p, and probably also of MYCN amplification.
机译:在对154个神经母细胞瘤的研究中,在1p(13%,19/143),11q(19%,11/59),14q(15%,15/97),17p(5%)上观察到杂合性(LOH)丧失,5/105)和17q(17%,9/52)。我们还发现14%(13/95)的神经母细胞瘤中NM23H1拷贝数增加。除一个拷贝数增加的肿瘤外,所有肿瘤均用抗NM23H1单克隆抗体染色为阳性。 19例1p LOH患者的无事件生存(EFS)明显少于128例无事件生存(41%vs 77%的4年EFS,P = 0.0093),以及13例NM23H1拷贝数增加的患者比82例正常基因的拷贝数(61%vs 84%的4年EFS,P = 0.0103)。 11q,14q或17q上的LOH不会影响EFS。 LOH≥1p,NM23H1拷贝数增加或MYCN扩增的大多数肿瘤发生在12个月或以上的患者,患有晚期疾病的患者以及显示接近二倍体或假二倍体的患者。但是,在NM23H1拷贝数增加的13个肿瘤中,只有1p出现了LOH,而在另外一个这样的肿瘤中,MYCN扩增了4个拷贝。这些发现表明,NM23H1拷贝数的增加可能是预后不良的预测因素,与1p的LOH无关,也可能与MYCN扩增无关。

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