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新型内皮素转换酶基因Nbla03145/ECEL1α和β的高表达与人神经母细胞瘤的良好预后相关。

High expression of the novel endothelin-converting enzyme genes, Nbla03145/ECEL1alpha and beta, is associated with favorable prognosis in human neuroblastomas.

作者信息

Kawamoto T, Ohira M, Hamano S, Hori T, Nakagawara A

机构信息

Division of Biochemistry, Chiba Cancer Center Research Institute, Chiba 260-8717, Japan.

出版信息

Int J Oncol. 2003 Apr;22(4):815-22.

Abstract

The clinicobiological feature of neuroblastoma is enigmatic because spontaneous regression often occurs in early stages of tumors of the patients under 1 year of age, while rapid growth usually occurs in the tumors of the patients over 1 year of age. Such difference in the clinical behavior may be caused by the difference in the pattern of gene expression among the subsets of neuroblastoma. To understand the molecular basis of neuroblastoma biology, we decided to identify the novel genes expressed differentially between favorable and unfavorable neuroblastomas. The oligo-capping cDNA libraries were constructed from different subsets of neuroblastomas. After random selection and DNA sequencing, the differentially expressed genes between favorable and unfavorable neuroblastomas were screened by reverse transcriptase-PCR. The clinical significance of gene expression was evaluated based on the results of Northern blot analysis. We have identified a novel gene Nbla03145 (alpha), also cloned and termed by another group as ECEL1, which encodes a new member of putative zinc-binding metalloendopeptidase (endothelin-converting enzyme) with unknown substrate. We also cloned a COOH-terminally truncated Nbla03145/ECEL1beta which is expressed only in thymus. In primary NBLs, the alpha isoform is more preferentially expressed than the beta isoform. High levels of Nbla03145/ECEL1 expression were significantly correlated with a younger age (p=0.0005), lower stages (p=0.0019), high level of TrkA expression (p</=0.00005), a single copy of MYCN (p<0.00005) and the tumors found by mass screening (p<0.00005). Decreased expression of Nbla03145/ECEL1 mRNA was significantly associated with poor prognosis (log-rank test: p=0.012). The present results have shown that expression of Nbla03145/ECEL1 is a novel prognostic marker of neuroblastoma. Further analysis of the gene may also give a cue to the understanding of the role of endothelin-like signaling in neuroblastoma and to the development of diagnostic and therapeutic strategies against aggressive tumors.

摘要

神经母细胞瘤的临床生物学特征令人费解,因为1岁以下患者的肿瘤在早期阶段常出现自发消退,而1岁以上患者的肿瘤通常快速生长。临床行为的这种差异可能是由神经母细胞瘤亚群间基因表达模式的差异所导致。为了解神经母细胞瘤生物学的分子基础,我们决定鉴定在预后良好和预后不良的神经母细胞瘤之间差异表达的新基因。从神经母细胞瘤的不同亚群构建了寡聚帽cDNA文库。经过随机选择和DNA测序后,通过逆转录聚合酶链反应筛选预后良好和预后不良的神经母细胞瘤之间差异表达的基因。基于Northern印迹分析结果评估基因表达的临床意义。我们鉴定出一个新基因Nbla03145(α),另一研究组也对其进行了克隆并命名为ECEL1,它编码一种底物未知的假定锌结合金属内肽酶(内皮素转换酶)新成员。我们还克隆了一个仅在胸腺中表达的COOH末端截短的Nbla03145/ECEL1β。在原发性神经母细胞瘤中,α异构体比β异构体更优先表达。高水平的Nbla03145/ECEL1表达与较年轻的年龄(p=0.0005)、较低的分期(p=0.0019)、高水平的TrkA表达(p≤0.00005)、MYCN单拷贝(p<0.00005)以及通过群体筛查发现的肿瘤(p<0.00005)显著相关。Nbla03145/ECEL1 mRNA表达降低与预后不良显著相关(对数秩检验:p=0.012)。目前的结果表明,Nbla03145/ECEL1的表达是神经母细胞瘤一种新的预后标志物。对该基因的进一步分析也可能为理解内皮素样信号在神经母细胞瘤中的作用以及针对侵袭性肿瘤的诊断和治疗策略的开发提供线索。

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