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High-throughput loss-of-heterozygosity study of chromosome 3p in lung cancer using single-nucleotide polymorphism markers

机译:使用单核苷酸多态性标记物对肺癌中染色体3p的高通量杂合性丢失研究

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摘要

Loss of DNA copy number at the short arm of chromosome 3 is one of the most common genetic changes in human lung cancer, suggesting the existence of one or more tumor suppressor genes (TSG) at 3p. To identify most frequently deleted regions and candidate TSGs within these regions, a recently developed single-nucleotide polymorphism (SNP)-mass spectrometry-genotyping (SMSG) technology was applied to investigate the loss of heterozygosity (LOH) in 30 primary non-small-cell lung cancers. A total of 386 SNP markers that spanned a region of 70 Mb at 3p, from 3pter to 3p14.1, were selected for LOH analysis. The average intermarker distance in the present study is ∼180 kb. Several frequently deleted regions, including 3p26.3, 3p25.3, 3p24.1, 3p23, and 3p21.1, were found. Several candidate TSGs within these frequently detected LOH regions have been found, including APG7L at 3p25.3, CLASP2 at 3p23, and CACNA2D3 at 3p21.1. This study also showed that SMSG technology is a very useful approach to rapidly define the minimal deleted region and to identify target TSGs in a given cancer. ©2006 American Association for Cancer Research.
机译:DNA拷贝数在3号染色体短臂上的丢失是人类肺癌中最常见的遗传变化之一,表明在3p处存在一个或多个肿瘤抑制基因(TSG)。为了识别这些区域中最常删除的区域和候选TSG,最近使用了一种新开发的单核苷酸多态性(SNP)-质谱-基因分型(SMSG)技术来研究30个主要非小基因小鼠中杂合性(LOH)的丧失。细胞肺癌。总共386个SNP标记在3p范围从3pter到3p14.1跨越了70 Mb区域,用于LOH分析。在本研究中,平均标记间距离约为180 kb。找到了几个经常删除的区域,包括3p26.3、3p25.3、3p24.1、3p23和3p21.1。在这些经常检测到的LOH区域中发现了几个候选TSG,包括3p25.3处的APG7L,3p23处的CLASP2和3p21.1处的CACNA2D3。这项研究还表明,SMSG技术是一种非常有用的方法,可以快速定义最小缺失区域并确定给定癌症中的目标TSG。 ©2006美国癌症研究协会。

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