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神经元特异性hel-N1和HuD作为神经母细胞瘤的新型分子标志物:HuD信使核糖核酸水平与良好预后特征的相关性

Neuron-specific hel-N1 and HuD as novel molecular markers of neuroblastoma: a correlation of HuD messenger RNA levels with favorable prognostic features.

作者信息

Ball N S, King P H

机构信息

Laboratory of Medical Genetics and Department of Neurology, University of Alabama, Birmingham, Alabama 35294, USA.

出版信息

Clin Cancer Res. 1997 Oct;3(10):1859-65.

PMID:9815574
Abstract

Hel-N1 and HuD belong to the elav gene family and encode neuron-specific RNA-binding proteins that are temporally regulated in neural development. Recently, these genes have been detected in small cell lung carcinoma, a neuroendocrine tumor, with HuD down-regulated in poorly differentiated, variant subsets. We, therefore, sought to determine: (a) the extent to which Hel-N1 and HuD are expressed in neuroblastoma (NB); and (b) whether the individual patterns of expression are associated with clinical features of the tumor. We used a sensitive and quantitative RNase protection assay that reliably distinguishes between these homologous genes, and with it we show that Hel-N1 and HuD transcripts were detected in 100% of cultured cells (11 of 11) and 97% of primary tumor samples (35 of 36). Densitometric quantification of transcripts indicated that the levels of HuD and Hel-N1 varied in all samples. In primary NB tissue, samples that expressed the highest Hel-N1 or HuD levels were N-myc unamplified. With HuD, the level in unamplified primary tumors was significantly higher than that of amplified tumors (0.80 +/- 0.12 versus 0.33 +/- 0.12, P < 0.02). HuD expression in prognostically favorable tumor stages was also significantly higher than unfavorable stages (0.98 +/- 0.19 versus 0.47 +/- 0.08, P < 0.03). In summary, the ubiquitous detection of HuD and Hel-N1 in NB indicates that they are molecular neuronal markers of this tumor. Furthermore, high HuD mRNA levels may predict a clinically favorable outcome.

摘要

Hel-N1和HuD属于elav基因家族,编码在神经发育过程中受到时间调控的神经元特异性RNA结合蛋白。最近,在神经内分泌肿瘤小细胞肺癌中检测到了这些基因,在低分化、变异亚群中HuD表达下调。因此,我们试图确定:(a) Hel-N1和HuD在神经母细胞瘤(NB)中的表达程度;(b) 个体表达模式是否与肿瘤的临床特征相关。我们使用了一种灵敏的定量核糖核酸酶保护分析方法,该方法能可靠地区分这些同源基因,结果显示在100%的培养细胞(11个样本中的11个)和97%的原发性肿瘤样本(36个样本中的35个)中检测到了Hel-N1和HuD转录本。转录本的密度定量分析表明,所有样本中HuD和Hel-N1的水平各不相同。在原发性NB组织中,Hel-N1或HuD表达水平最高的样本N-myc未扩增。对于HuD,未扩增原发性肿瘤中的水平显著高于扩增肿瘤(0.80±0.12对0.33±0.12,P<0.02)。预后良好的肿瘤阶段中HuD的表达也显著高于预后不良阶段(0.98±0.19对0.47±0.08,P<0.03)。总之,在NB中普遍检测到HuD和Hel-N1表明它们是该肿瘤的分子神经元标志物。此外,高HuD mRNA水平可能预示着临床预后良好。

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