Momand J, Jung D, Wilczynski S, Niland J
Department of Cell and Tumor Biology, Beckman Research Institute, National Medical Center, 1450 East Duarte Road, Duarte, CA 91010-3000, USA.
Nucleic Acids Res. 1998 Aug 1;26(15):3453-9. doi: 10.1093/nar/26.15.3453.
The p53 tumor suppressor gene is inactivated in human tumors by several distinct mechanisms. The best characterized inactivation mechanisms are: (i) gene mutation; (ii) p53 protein association with viral proteins; (iii) p53 protein association with the MDM2 cellular oncoprotein. The MDM2 gene has been shown to be abnormally up-regulated in human tumors and tumor cell lines by gene amplification, increased transcript levels and enhanced translation. This communication presents a brief review of the spectrum of MDM2 abnormalities in human tumors and compares the tissue distribution of MDM2 amplification and p53 mutation frequencies. In this study, 3889 samples from tumors or xenografts from 28 tumor types were examined for MDM2 amplification from previously published sources. The overall frequency of MDM2 amplification in these human tumors was 7%. Gene amplification was observed in 19 tumor types, with the highest frequency observed in soft tissue tumors (20%), osteosarcomas (16%) and esophageal carcinomas (13%). Tumors which showed a higher incidence of MDM2 amplification than p53 mutation were soft tissue tumors, testicular germ cell cancers and neuro-blastomas. Data from studies where both MDM2 amplification and p53 mutations were analyzed within the same samples showed that mutations in these two genes do not generally occur within the same tumor. In these studies, 29 out of a total of 33 MDM2 amplification-positive tumors had wild-type p53. We hypothesize that heretofore uncharacterized carcinogens favor MDM2 amplification over p53 mutations in certain tumor types. A database listing the MDM2 gene amplifications is available on the World Wide Web at http://www. infosci.coh.org/mdm2 . Charts of MDM2 amplification frequencies and comparisons with p53 genetic alterations are also available at this Web site.
p53肿瘤抑制基因在人类肿瘤中可通过多种不同机制失活。目前已明确的失活机制有:(i)基因突变;(ii)p53蛋白与病毒蛋白结合;(iii)p53蛋白与MDM2细胞癌蛋白结合。研究表明,MDM2基因在人类肿瘤和肿瘤细胞系中通过基因扩增、转录水平增加及翻译增强而异常上调。本文简要综述了人类肿瘤中MDM2异常的情况,并比较了MDM2扩增和p53突变频率的组织分布。在本研究中,从先前发表的资料中选取了来自28种肿瘤类型的肿瘤或异种移植物的3889个样本,检测MDM2扩增情况。这些人类肿瘤中MDM2扩增的总体频率为7%。在19种肿瘤类型中观察到基因扩增,其中软组织肿瘤(20%)、骨肉瘤(16%)和食管癌(13%)的扩增频率最高。MDM2扩增发生率高于p53突变的肿瘤有软组织肿瘤、睾丸生殖细胞癌和神经母细胞瘤。在同一样本中同时分析MDM2扩增和p53突变的研究数据表明,这两个基因的突变通常不在同一肿瘤中发生。在这些研究中,33个MDM2扩增阳性肿瘤中共有29个具有野生型p53。我们推测,迄今为止未明确的致癌物在某些肿瘤类型中更倾向于导致MDM2扩增而非p53突变。可通过万维网(http://www.infosci.coh.org/mdm2)获取列出MDM2基因扩增情况的数据库。该网站还提供MDM2扩增频率图表以及与p53基因改变的比较。