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低级别和高级别骨肉瘤中12号染色体序列的差异扩增

Differentially amplified chromosome 12 sequences in low- and high-grade osteosarcoma.

作者信息

Gisselsson David, Pålsson Eva, Höglund Mattias, Domanski Henryk, Mertens Fredrik, Pandis Nikos, Sciot Raf, Dal Cin Paola, Bridge Julia A, Mandahl Nils

机构信息

Department of Clinical Genetics, University Hospital, Lund, Sweden.

出版信息

Genes Chromosomes Cancer. 2002 Feb;33(2):133-40. doi: 10.1002/gcc.1219.

Abstract

Most osteosarcomas are highly aggressive malignancies characterized by a complex pattern of chromosome abnormalities. However, a subgroup of low-grade, parosteal tumors exhibits a relatively simple aberration pattern dominated by ring chromosomes carrying amplified material from chromosome 12. To assess whether sequences from this chromosome were differentially amplified in low- and high-grade osteosarcomas, copy numbers of the CCND2, ETV6, KRAS2, and D12S85 regions in 12p and the MDM2 region in 12q were evaluated by interphase or metaphase fluorescence in situ hybridization (FISH) in 24 osteosarcomas. Amplification of MDM2 was detected in all five low-grade and four high-grade osteosarcomas, all of which showed ring chromosomes. An overrepresentation of 12p sequences was found in 1/5 low-grade and in 9/19 high-grade tumors. Multicolor single-copy FISH analysis of metaphase cells from six high-grade tumors showed that extra 12p material either occurred together with MDM2 in ring chromosomes or was scattered over the genome as a result of complex structural rearrangements. Most tumors (8/10) not containing amplification of the assessed chromosome 12 loci exhibited a nondiploid pattern at evaluation with probes for centromeric alpha satellite sequences. These findings indicate that gain of sequences from the short arm of chromosome 12 could be a possible genetic pathway in the development of aggressive osteosarcoma.

摘要

大多数骨肉瘤是具有高度侵袭性的恶性肿瘤,其特征是染色体异常模式复杂。然而,一组低级别骨膜外肿瘤表现出相对简单的畸变模式,以携带12号染色体扩增物质的环状染色体为主。为了评估该染色体的序列在低级别和高级别骨肉瘤中是否存在差异扩增,通过间期或中期荧光原位杂交(FISH)对24例骨肉瘤中12p上的CCND2、ETV6、KRAS2和D12S85区域以及12q上的MDM2区域的拷贝数进行了评估。在所有5例低级别骨肉瘤和4例高级别骨肉瘤中均检测到MDM2扩增,所有这些肿瘤均显示环状染色体。在1/5的低级别肿瘤和9/19的高级别肿瘤中发现12p序列的过度表达。对6例高级别肿瘤的中期细胞进行多色单拷贝FISH分析表明,额外的12p物质要么与MDM2一起出现在环状染色体中,要么由于复杂的结构重排而散布在基因组中。大多数(8/10)未检测到评估的12号染色体位点扩增的肿瘤在用着丝粒α卫星序列探针评估时表现出非二倍体模式。这些发现表明,12号染色体短臂序列的增加可能是侵袭性骨肉瘤发生发展中的一条可能的遗传途径。

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