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肝母细胞瘤与相应正常肝脏之间的表达谱分析及差异筛选:鉴定PLK1癌基因的高表达作为肝母细胞瘤预后不良的指标

Expression profiling and differential screening between hepatoblastomas and the corresponding normal livers: identification of high expression of the PLK1 oncogene as a poor-prognostic indicator of hepatoblastomas.

作者信息

Yamada Shin-ichi, Ohira Miki, Horie Hiroshi, Ando Kiyohiro, Takayasu Hajime, Suzuki Yutaka, Sugano Sumio, Hirata Takahiro, Goto Takeshi, Matsunaga Tadashi, Hiyama Eiso, Hayashi Yutaka, Ando Hisami, Suita Sachiyo, Kaneko Michio, Sasaki Fumiaki, Hashizume Kohei, Ohnuma Naomi, Nakagawara Akira

机构信息

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

出版信息

Oncogene. 2004 Aug 5;23(35):5901-11. doi: 10.1038/sj.onc.1207782.

Abstract

Hepatoblastoma is one of the most common malignant liver tumors in young children. Recent evidences have suggested that the abnormalities in Wnt signaling pathway, as seen in frequent mutation of the beta-catenin gene, may play a role in the genesis of hepatoblastoma. However, the precise mechanism to cause the tumor has been elusive. To identify novel hepatoblastoma-related genes for unveiling the molecular mechanism of the tumorigenesis, a large-scale cloning of cDNAs and differential screening of their expression between hepatoblastomas and the corresponding normal livers were performed. We constructed four full-length-enriched cDNA libraries using an oligo-capping method from the primary tissues which included two hepatoblastomas with high levels of alpha-fetoprotein (AFP), a hepatoblastoma without production of AFP, and a normal liver tissue corresponded to the tumor. Among the 10,431 cDNAs randomly picked up and successfully sequenced, 847 (8.1%) were the genes with unknown function. Of interest, the expression profile among the two subsets of hepatoblastoma and a normal liver was extremely different. A semiquantitative RT-PCR analysis showed that 86 out of 1188 genes tested were differentially expressed between hepatoblastomas and the corresponding normal livers, but that only 11 of those were expressed at high levels in the tumors. Notably, PLK1 oncogene was expressed at very high levels in hepatoblastomas as compared to the normal infant's livers. Quantitative real-time RT-PCR analysis for the PLK1 mRNA levels in 74 primary hepatoblastomas and 29 corresponding nontumorous livers indicated that the patients with hepatoblastoma with high expression of PLK1 represented significantly poorer outcome than those with its low expression (5-year survival rate: 55.9 vs 87.0%, respectively, p=0.042), suggesting that the level of PLK1 expression is a novel marker to predict the prognosis of hepatoblastoma. Thus, the differentially expressed genes we have identified may become a useful tool to develop new diagnostic as well as therapeutic strategies of hepatoblastoma.

摘要

肝母细胞瘤是幼儿最常见的恶性肝脏肿瘤之一。最近的证据表明,Wnt信号通路异常,如β-连环蛋白基因频繁突变,可能在肝母细胞瘤的发生中起作用。然而,导致肿瘤的确切机制一直难以捉摸。为了鉴定与肝母细胞瘤相关的新基因以揭示肿瘤发生的分子机制,我们进行了大规模的cDNA克隆以及肝母细胞瘤与其相应正常肝脏之间的表达差异筛选。我们使用寡聚帽法从包括两个甲胎蛋白(AFP)水平高的肝母细胞瘤、一个不产生AFP的肝母细胞瘤以及与肿瘤对应的正常肝脏组织的原始组织构建了四个全长富集cDNA文库。在随机挑选并成功测序的10431个cDNA中,847个(8.1%)是功能未知的基因。有趣的是,肝母细胞瘤的两个亚组与正常肝脏之间的表达谱差异极大。半定量RT-PCR分析表明,在检测的1188个基因中,有86个在肝母细胞瘤与其相应正常肝脏之间差异表达,但其中只有11个在肿瘤中高水平表达。值得注意的是,与正常婴儿肝脏相比,PLK1癌基因在肝母细胞瘤中表达水平非常高。对74例原发性肝母细胞瘤和29例相应的非肿瘤性肝脏中PLK1 mRNA水平进行的定量实时RT-PCR分析表明,PLK1高表达的肝母细胞瘤患者的预后明显比低表达患者差(5年生存率分别为55.9%和87.0%,p = 0.042),这表明PLK1表达水平是预测肝母细胞瘤预后的一个新标志物。因此,我们鉴定出的差异表达基因可能成为开发肝母细胞瘤新诊断和治疗策略的有用工具。

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