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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >The polyamine metabolism genes ornithine decarboxylase and antizyme 2 predict aggressive behavior in neuroblastomas with and without MYCN amplification.
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The polyamine metabolism genes ornithine decarboxylase and antizyme 2 predict aggressive behavior in neuroblastomas with and without MYCN amplification.

机译:多胺代谢基因鸟氨酸脱羧酶和抗酶2预测在有和没有MYCN扩增的神经母细胞瘤中的攻击行为。

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摘要

High polyamine (PA) levels and ornithine decarboxylase (ODC) overexpression are well-known phenomena in many aggressive cancer types. We analyzed the expression of ODC and ODC-activity regulating genes antizymes 1-3 (OAZ1-3) and antizyme inhibitors 1-2 (AZ-IN1-2) in human neuroblastoma (NB) tumors and correlated these with genetic and clinical features of NB. Since ODC is a known target gene of MYCN, the correlation between ODC and MYCN was of special interest. Data were obtained from Affymetrix micro-array analysis of 88 NB tumor samples. In addition, mRNA expression levels of ODC, OAZ2 and MYCN in a MYCN-inducible NB cell line were determined by quantitative real-time reverse-transcriptase polymerase chain reaction (RT-PCR). ODC mRNA expression in NB tumors was significantly predictive of decreased overall survival probability and correlated with several unfavorable clinical NB characteristics (all p < 0.005). Interestingly, high ODC mRNA expression also showed significant correlation with poor survival prognosis in Kaplan-Meier analyses stratified for patients without MYCN amplification, suggesting an additional role for ODC independent of MYCN. Conversely, high OAZ2 mRNA expression correlated with increased survival and with several favorable clinical NB characteristics (all p < 0.003). In addition, we provide first evidence of a role for MYCN-associated transcription factors MAD2 and MAD7 in ODC regulation. In NB cell cultures, ectopic overexpression of MYCN altered ODC but not OAZ2 mRNA levels. In conclusion, these data suggest that elevated ODC and low OAZ2 mRNA expression levels correlate with several unfavorable genetic and clinical features in NB, offering new insights into PA pathways and PA metabolism-targeting therapy in NB.
机译:高多胺(PA)水平和鸟氨酸脱羧酶(ODC)过表达是许多侵袭性癌症类型中的众所周知的现象。我们分析了ODC和ODC活性调节基因抗酶1-3(OAZ1-3)和抗酶抑制剂1-2(AZ-IN1-2)在人神经母细胞瘤(NB)肿瘤中的表达,并将其与人神经母细胞瘤(NB)的遗传和临床特征相关联注意由于ODC是MYCN的已知靶基因,因此ODC与MYCN之间的相关性特别令人关注。数据从88个NB肿瘤样品的Affymetrix微阵列分析获得。另外,通过定量实时逆转录酶聚合酶链反应(RT-PCR)确定在MYCN诱导的NB细胞系中ODC,OAZ2和MYCN的mRNA表达水平。 NB肿瘤中的ODC mRNA表达可显着预测整体存活率降低,并与几种不良的NB临床特征相关(所有p <0.005)。有趣的是,在没有MYCN扩增的患者中进行分层的Kaplan-Meier分析中,高ODC mRNA表达还显示出不良的预后,这也暗示了ODC的独立作用。相反,高OAZ2 mRNA表达与增加的生存率和一些良好的临床NB特征相关(所有p <0.003)。此外,我们提供了MYCN相关转录因子MAD2和MAD7在ODC调节中的作用的第一个证据。在NB细胞培养物中,MYCN的异位过表达改变了ODC,但没有改变OAZ2 mRNA的水平。总之,这些数据表明,ODC升高和OAZ2 mRNA低表达与NB的一些不良遗传和临床特征相关,从而为NB中的PA途径和PA代谢靶向疗法提供了新见解。

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