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MYCN扩增子的共扩增模式是大多数MYCN扩增的人类神经母细胞瘤的一个不变特征。

The coamplification pattern of the MYCN amplicon is an invariable attribute of most MYCN-amplified human neuroblastomas.

作者信息

Weber Axel, Starke Sven, Bergmann Eckhard, Christiansen Holger

机构信息

Children's Hospital, Pediatric Hematology and Oncology, University of Marburg, Marburg, Germany.

出版信息

Clin Cancer Res. 2006 Dec 15;12(24):7316-21. doi: 10.1158/1078-0432.CCR-06-0837.

DOI:10.1158/1078-0432.CCR-06-0837
PMID:17189403
Abstract

PURPOSE

Fifteen percent to 20% of human neuroblastomas show amplification of the MYCN oncogene physiologically located at chromosome 2p24-25, indicating an aggressive subtype of human neuroblastoma with a poor clinical outcome. Recent findings revealed that the structure of the amplicon differs interindividually and that coamplification of genes in telomeric proximity to MYCN might play a relevant role in neuroblastoma development and response to treatment, respectively. We now asked if the amplicon structure is an invariable attribute of an individual tumor or if the coamplification pattern could change during progress or in case of recurrent disease.

EXPERIMENTAL DESIGN

We used a previously described multiplex PCR approach to analyze the coamplification status of MYCN-amplified human neuroblastomas (n = 33) in tumor tissue at the time of initial diagnosis and in consecutive tissue specimens at later time points after initial treatment or from relapsing disease. The MYCN copy number per haploid genome (Mcn/hg) in these specimens was determined in a separate duplex PCR.

RESULTS

In 32 of the 33 investigated tumors, the amplicon structure showed no changes after initial chemotherapy and in recurrent disease. Mcn/hg showed a decrease after initial treatment (n = 23), whereas we found a significant increase in recurrent disease (n = 10).

CONCLUSION

Our data indicate that the initial determined structure of the 2p24-25 amplicon is a consistent attribute in the great majority of the individual MYCN-amplified neuroblastomas and shows no plasticity during or after chemotherapy. Observed changes in the Mcn/hg over the course of disease are in line with preexisting cell culture findings.

摘要

目的

15%至20%的人类神经母细胞瘤显示位于染色体2p24 - 25上的MYCN癌基因发生扩增,这表明人类神经母细胞瘤的一种侵袭性亚型,临床预后较差。最近的研究发现,扩增子的结构在个体间存在差异,并且在MYCN端粒附近的基因共扩增可能分别在神经母细胞瘤的发生发展和对治疗的反应中发挥相关作用。我们现在要问,扩增子结构是单个肿瘤的一个不变属性,还是共扩增模式在疾病进展过程中或复发性疾病时会发生变化。

实验设计

我们使用先前描述的多重PCR方法,分析初诊时肿瘤组织中以及初始治疗后较晚时间点或复发性疾病的连续组织标本中MYCN扩增的人类神经母细胞瘤(n = 33)的共扩增状态。在单独的双重PCR中测定这些标本中单倍体基因组的MYCN拷贝数(Mcn/hg)。

结果

在33个研究的肿瘤中,有32个在初始化疗后和复发性疾病中扩增子结构未显示变化。初始治疗后Mcn/hg显示下降(n = 23),而我们发现在复发性疾病中有显著增加(n = 10)。

结论

我们的数据表明,2p24 - 25扩增子的初始确定结构在大多数个体MYCN扩增的神经母细胞瘤中是一个一致的属性,并且在化疗期间或化疗后没有可塑性。在疾病过程中观察到的Mcn/hg变化与先前细胞培养的结果一致。

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