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一种用于比较肿瘤学的全基因组方法:犬类和人类骨肉瘤的高分辨率寡核苷酸阵列比较基因组杂交确定了共同的微畸变。

A genome-wide approach to comparative oncology: high-resolution oligonucleotide aCGH of canine and human osteosarcoma pinpoints shared microaberrations.

作者信息

Angstadt Andrea Y, Thayanithy Venugopal, Subramanian Subbaya, Modiano Jaime F, Breen Matthew

机构信息

Department of Molecular Biomedical Sciences, North Carolina State University, Raleigh, NC, USA.

出版信息

Cancer Genet. 2012 Nov;205(11):572-87. doi: 10.1016/j.cancergen.2012.09.005. Epub 2012 Nov 6.

DOI:10.1016/j.cancergen.2012.09.005
PMID:23137772
Abstract

Molecular cytogenetic evaluation of human osteosarcoma (OS) has revealed the characteristically high degree of genomic reorganization that is the hallmark of this cancer. The extent of genomic disorder in OS has hindered identification of the genomic aberrations driving disease progression. With pathophysiological similarities to its human counterpart, canine OS represents an ideal model for comparison of conserved regions of genomic instability that may be disease-associated rather than genomic passengers. This study used high-resolution oligonucleotide array comparative genomic hybridization and a variety of informatics tools to aid in the identification of disease-associated genome-wide DNA copy number aberrations in canine and human OS. Our findings support and build upon the high level of cytogenetic complexity, through the identification of shared regions of microaberration (<500 kb) and functional analysis of possible orthologous OS-associated genes to pinpoint the cellular processes most commonly affected by aberration in human and canine OS. Aberrant regions contained previously reported genes such as CDC5L, MYC, RUNX2, and CDKN2A/CDKN2B, while expanding the gene of interest list to include ADAM15, CTC1, MEN1, CDK7, and others. Such regions of instability may thus have functional significance in the etiology of OS, the most common primary bone tumor in both species.

摘要

对人类骨肉瘤(OS)的分子细胞遗传学评估显示,其具有典型的高度基因组重组现象,这是该癌症的标志。骨肉瘤中基因组紊乱的程度阻碍了对驱动疾病进展的基因组畸变的识别。犬类骨肉瘤在病理生理学上与人类骨肉瘤相似,是比较可能与疾病相关而非基因组过客的基因组不稳定保守区域的理想模型。本研究使用高分辨率寡核苷酸阵列比较基因组杂交技术和各种信息学工具,以帮助识别犬类和人类骨肉瘤中与疾病相关的全基因组DNA拷贝数畸变。我们的研究结果通过识别微畸变共享区域(<500 kb)以及对可能的直系同源骨肉瘤相关基因进行功能分析,来确定人类和犬类骨肉瘤中最常受畸变影响的细胞过程,从而支持并进一步证实了细胞遗传学复杂性的高水平。异常区域包含先前报道的基因,如CDC5L、MYC、RUNX2和CDKN2A/CDKN2B,同时扩大了感兴趣基因列表,包括ADAM15、CTC1、MEN1、CDK7等。因此,这种不稳定区域可能在骨肉瘤(这两个物种中最常见的原发性骨肿瘤)的病因学中具有功能意义。

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