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Microarray comparative genomic hybridisation analysis of intraocular uveal melanomas identifies distinctive imbalances associated with loss of chromosome 3

机译:眼葡萄膜黑色素瘤的微阵列比较基因组杂交分析确定了与3号染色体丢失相关的独特失衡

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摘要

Defining regions of genomic imbalance can identify genes involved in tumour development. Conventional cytogenetics has identified several nonrandom copy number alterations (CNA) in uveal melanomas (UVM), which include monosomy 3, chromosome 6 abnormalities and gain of 8q. To gain further insight into the CNAs and define the regions involved more precisely we analysed 18 primary UVMs using 1 Mb BAC microarray comparative genomic hybridisation (CGH). Our analysis showed that the most common genomic imbalances were 8q gain (78%), 6p gain (67%) and monosomy 3 (56%). Two distinct CGH profiles could be delineated on the basis of the chromosome 3 status. The most common genetic changes in monosomy 3 tumours, in our study, were gain of 8q11.21–q24.3, 6p25.1–p21.2, 21q21.2–q21.3 and 21q22.13–q22.3 and loss of 1p36.33–p34.3, 1p31.1–p21.2, 6q16.2–q25.3 and 8p23.3–p11.23. In contrast, disomy 3 tumours showed recurrent gains of only 6p25.3–p22.3 and 8q23.2–q24.3. Our approach allowed definition of the smallest overlapping regions of imbalance, which may be important in the development of UVM.
机译:定义基因组失衡区域可以鉴定参与肿瘤发展的基因。传统的细胞遗传学已经确定了葡萄膜黑色素瘤(UVM)中的几种非随机拷贝数改变(CNA),包括单核3、6号染色体异常和8q增益。为了进一步了解CNA并更准确地定义涉及的区域,我们使用1 Mb BAC微阵列比较基因组杂交(CGH)分析了18种主要UVM。我们的分析表明,最常见的基因组失衡是8q增益(78%),6p增益(67%)和3号单体(56%)。根据3号染色体的状态,可以描绘出两个不同的CGH图谱。在我们的研究中,最常见的3体肿瘤遗传改变是8q11.21–q24.3、6p25.1–p21.2、21q21.2–q21.3和21q22.13–q22.3 1p36.33–p34.3、1p31.1–p21.2、6q16.2–q25.3和8p23.3–p11.23的值。相比之下,二三体肿瘤的复发率仅为6p25.3–p22.3和8q23.2–q24.3。我们的方法允许定义不平衡的最小重叠区域,这在UVM的开发中可能很重要。

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