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人类恶性胶质瘤中12q13 - q15扩增子的精细定位表明CDK4/SAS和MDM2是独立的扩增靶点。

Refined mapping of 12q13-q15 amplicons in human malignant gliomas suggests CDK4/SAS and MDM2 as independent amplification targets.

作者信息

Reifenberger G, Ichimura K, Reifenberger J, Elkahloun A G, Meltzer P S, Collins V P

机构信息

Department of Neuropathology, Heinrich Heine University, Düsseldorf, Germany.

出版信息

Cancer Res. 1996 Nov 15;56(22):5141-5.

PMID:8912848
Abstract

We have reported previously that about 15% of anaplastic astrocytomas and glioblastomas show amplification and overexpression of one or more genes from chromosomal segment 12q13-q15 (G. Reifenberger et al., Cancer Res., 54, 4299-4303, 1994). The genes most frequently amplified and overexpressed were CDK4 (with coamplification of SAS) and MDM2. Because individual malignant gliomas showed CDK4/SAS amplification but no MDM2 amplification and vice versa, the possibility remained of a common amplification target gene located between CDK4 and MDM2. We have addressed this question by performing a detailed amplicon mapping of a series of 24 primary malignant gliomas and two glioblastoma cell lines with 12q13-q15 amplification. All tumors and cell lines were analyzed at eight gene loci and six anonymous loci from 12q13-q15, including seven loci located between CDK4 and MDM2. These studies revealed two centers of amplification, one at CDK4/SAS and the other at MDM2. A number of loci located close to either MDM2 or CDK4/SAS, including the genes GADD153, GLI, RAP1B, A2MR, and IFNG, were found to be coamplified in some tumors but not overexpressed consistently. All amplicons were discontinuous between CDK4/SAS and MDM2. Our results thus exclude a common amplification target between CDK4/SAS and MDM2 and provide additional evidence that these genes represent two independent targets of selection.

摘要

我们先前已报道,约15%的间变性星形细胞瘤和胶质母细胞瘤显示出12号染色体13区至15区(G. Reifenberger等人,《癌症研究》,54卷,4299 - 4303页,1994年)的一个或多个基因发生扩增和过表达。最常发生扩增和过表达的基因是CDK4(伴有SAS共扩增)和MDM2。由于个别恶性胶质瘤显示出CDK4/SAS扩增但无MDM2扩增,反之亦然,因此位于CDK4和MDM2之间存在一个共同扩增靶基因的可能性仍然存在。我们通过对一系列24例原发性恶性胶质瘤和两个具有12q13 - 15扩增的胶质母细胞瘤细胞系进行详细的扩增子图谱分析来解决这个问题。所有肿瘤和细胞系都在12q13 - 15的八个基因位点和六个匿名位点进行了分析,包括位于CDK4和MDM2之间的七个位点。这些研究揭示了两个扩增中心,一个在CDK4/SAS,另一个在MDM2。发现一些靠近MDM2或CDK4/SAS的位点,包括GADD153、GLI、RAP1B、A2MR和IFNG基因,在一些肿瘤中发生了共扩增,但并非始终过表达。所有扩增子在CDK4/SAS和MDM2之间都是不连续的。因此,我们的结果排除了CDK4/SAS和MDM2之间存在共同扩增靶标的可能性,并提供了额外的证据表明这些基因代表两个独立的选择靶标。

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