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新型非编码RNA MALAT-1和胸腺素β4可预测早期非小细胞肺癌的转移和生存情况。

MALAT-1, a novel noncoding RNA, and thymosin beta4 predict metastasis and survival in early-stage non-small cell lung cancer.

作者信息

Ji Ping, Diederichs Sven, Wang Wenbing, Böing Sebastian, Metzger Ralf, Schneider Paul M, Tidow Nicola, Brandt Burkhard, Buerger Horst, Bulk Etmar, Thomas Michael, Berdel Wolfgang E, Serve Hubert, Müller-Tidow Carsten

机构信息

Department of Medicine, University of Münster, Germany.

出版信息

Oncogene. 2003 Sep 11;22(39):8031-41. doi: 10.1038/sj.onc.1206928.

Abstract

Early-stage non-small cell lung cancer (NSCLC) can be cured by surgical resection, but a substantial fraction of patients ultimately dies due to distant metastasis. In this study, we used subtractive hybridization to identify gene expression differences in stage I NSCLC tumors that either did or did not metastasize in the course of disease. Individual clones (n=225) were sequenced and quantitative RT-PCR verified overexpression in metastasizing samples. Several of the identified genes (eIF4A1, thymosin beta4 and a novel transcript named MALAT-1) were demonstrated to be significantly associated with metastasis in NSCLC patients (n=70). The genes' association with metastasis was stage- and histology specific. The Kaplan-Meier analyses identified MALAT-1 and thymosin beta4 as prognostic parameters for patient survival in stage I NSCLC. The novel MALAT-1 transcript is a noncoding RNA of more than 8000 nt expressed from chromosome 11q13. It is highly expressed in lung, pancreas and other healthy organs as well as in NSCLC. MALAT-1 expressed sequences are conserved across several species indicating its potentially important function. Taken together, these data contribute to the identification of early-stage NSCLC patients that are at high risk to develop metastasis. The identification of MALAT-1 emphasizes the potential role of noncoding RNAs in human cancer.

摘要

早期非小细胞肺癌(NSCLC)可通过手术切除治愈,但相当一部分患者最终会因远处转移而死亡。在本研究中,我们利用消减杂交技术来鉴定I期NSCLC肿瘤中在疾病过程中发生或未发生转移的基因表达差异。对单个克隆(n = 225)进行测序,并通过定量RT-PCR验证在发生转移的样本中的过表达情况。所鉴定的几个基因(eIF4A1、胸腺素β4和一个名为MALAT-1的新转录本)被证明与NSCLC患者(n = 70)的转移显著相关。这些基因与转移的关联具有阶段和组织学特异性。Kaplan-Meier分析确定MALAT-1和胸腺素β4为I期NSCLC患者生存的预后参数。新的MALAT-1转录本是一种从染色体11q13表达的超过8000 nt的非编码RNA。它在肺、胰腺和其他健康器官以及NSCLC中高表达。MALAT-1的表达序列在多个物种中保守,表明其可能具有重要功能。综上所述,这些数据有助于识别有高转移风险的早期NSCLC患者。MALAT-1的鉴定强调了非编码RNA在人类癌症中的潜在作用。

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