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人类胶质瘤中的基因扩增

Gene amplification in human gliomas.

作者信息

Collins V P

机构信息

Institute for Oncology and Pathology, Karolinska Institute, Stockholm, Sweden.

出版信息

Glia. 1995 Nov;15(3):289-96. doi: 10.1002/glia.440150309.

DOI:10.1002/glia.440150309
PMID:8586464
Abstract

Gliomas represent the largest group of primary brain tumors in adults. The astrocytic variants are the most common and the adult forms are histologically stratified into three malignancy grades. Of these glioblastoma is the most common and the most malignant; it has also been best studied by molecular genetics and cytogenetics. Double-minute chromosomes, known to represent amplified genes, are found in 50% of glioblastomas. Amplified genes are not detected in the most benign of the astrocytomas. Many genes have been shown to be amplified in more than single cases of gliomas and these include EGFR, CDK4, SAS, MDM2, GLI, PDGFAR, MYC, N MYC, MYCL1, MET, GADD153, and KIT. The most commonly amplified genes in glioblastomas are EGFR (in approximately 40%), CDK4, and SAS (in approximately 15%). The remainder of the genes are amplified at lower frequency. The best mapped amplicon in gliomas involves the 12q13-14 region. The amplicon is of undetermined size, encompasses a number of genes, and may be rearranged. It occurs in 15% of glioblastomas and almost always includes the CDK4 and SAS genes, in about 10% of tumors the MDM2 gene, and at lower frequency GLI, GADD153, and A2MR. All but A2MR are overexpressed if amplified. The amplified EGFR gene is frequently rearranged, resulting in changes in the regions of the transcript that codes for the extracellular domain. The resultant receptor is constitutively activated. These findings provide examples of the impact the use of modern molecular biological techniques has had on our understanding of oncogenic mechanisms in gliomas.

摘要

神经胶质瘤是成人原发性脑肿瘤中最大的一类。星形细胞变体最为常见,成人型在组织学上分为三个恶性等级。其中,胶质母细胞瘤最为常见且恶性程度最高;它也是分子遗传学和细胞遗传学研究得最透彻的。双微体染色体已知代表扩增基因,在50%的胶质母细胞瘤中可发现。在最良性的星形细胞瘤中未检测到扩增基因。许多基因已被证明在多例神经胶质瘤中扩增,这些基因包括表皮生长因子受体(EGFR)、细胞周期蛋白依赖性激酶4(CDK4)、SAS、小鼠双微体基因2(MDM2)、胶质瘤相关癌基因家族锌指蛋白(GLI)、血小板衍生生长因子受体α(PDGFAR)、原癌基因MYC、N-MYC、MYCL1、间质表皮转化因子(MET)、生长停滞和DNA损伤诱导蛋白153(GADD153)以及干细胞生长因子受体(KIT)。胶质母细胞瘤中最常扩增的基因是EGFR(约40%)、CDK4和SAS(约15%)。其余基因的扩增频率较低。神经胶质瘤中定位最好的扩增子涉及12q13 - 14区域。该扩增子大小不确定,包含多个基因,且可能发生重排。它出现在15%的胶质母细胞瘤中,几乎总是包括CDK4和SAS基因,约10%的肿瘤中包括MDM2基因,GLI、GADD153和A2MR基因的出现频率较低。除A2MR外,其他基因若扩增则会过度表达。扩增的EGFR基因经常发生重排,导致编码细胞外结构域的转录区域发生变化。由此产生的受体持续激活。这些发现为例证,说明了现代分子生物学技术的应用对我们理解神经胶质瘤致癌机制所产生的影响。

相似文献

1
Gene amplification in human gliomas.人类胶质瘤中的基因扩增
Glia. 1995 Nov;15(3):289-96. doi: 10.1002/glia.440150309.
2
Amplified genes in human gliomas.人类胶质瘤中的扩增基因。
Semin Cancer Biol. 1993 Feb;4(1):27-32.
3
Amplification of multiple genes from chromosomal region 12q13-14 in human malignant gliomas: preliminary mapping of the amplicons shows preferential involvement of CDK4, SAS, and MDM2.人类恶性胶质瘤中染色体区域12q13 - 14多个基因的扩增:扩增子的初步定位显示CDK4、SAS和MDM2优先受累。
Cancer Res. 1994 Aug 15;54(16):4299-303.
4
Refined mapping of 12q13-q15 amplicons in human malignant gliomas suggests CDK4/SAS and MDM2 as independent amplification targets.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。
Cancer Res. 1996 Nov 15;56(22):5141-5.
5
Amplification of KIT, PDGFRA, VEGFR2, and EGFR in gliomas.胶质瘤中KIT、PDGFRA、VEGFR2和EGFR的扩增
Mol Cancer Res. 2006 Dec;4(12):927-34. doi: 10.1158/1541-7786.MCR-06-0085.
6
Rarity of PTEN deletions and EGFR amplification in malignant gliomas of childhood: results from the Children's Cancer Group 945 cohort.儿童恶性胶质瘤中PTEN缺失和EGFR扩增的罕见性:儿童癌症组945队列研究结果
J Neurosurg. 2006 Nov;105(5 Suppl):418-24. doi: 10.3171/ped.2006.105.5.418.
7
Molecular analysis of the erbB gene family calmodulin-binding and calmodulin-like domains in astrocytic gliomas.星形胶质细胞瘤中erbB基因家族钙调蛋白结合域和类钙调蛋白域的分子分析
Int J Oncol. 2004 Nov;25(5):1489-94.
8
Mapping of amplification units in the q13-14 region of chromosome 12 in human sarcomas: some amplica do not include MDM2.人类肉瘤中12号染色体q13-14区域扩增单元的定位:一些扩增不包括MDM2。
Cell Growth Differ. 1993 Dec;4(12):1065-70.
9
p53 mutation, EGFR gene amplification and loss of heterozygosity on chromosome 10, 17 p in human gliomas.人类胶质瘤中的p53突变、表皮生长因子受体(EGFR)基因扩增以及10号和17号染色体短臂上的杂合性缺失
Chin Med J (Engl). 2000 Jul;113(7):662-6.
10
Gene amplification as a prognostic factor in primary and secondary high-grade malignant gliomas.基因扩增作为原发性和继发性高级别恶性胶质瘤的预后因素
Int J Oncol. 1998 Oct;13(4):717-24.

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