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与 HapMap Trios 相比,NCI-60 癌细胞系中大量纯合子的积累,以及与脆性位点定位的关系。

Mass homozygotes accumulation in the NCI-60 cancer cell lines as compared to HapMap Trios, and relation to fragile site location.

机构信息

Department of Health Sciences Research, Mayo Clinic College of Medicine, Rochester, Minnesota, United States of America.

出版信息

PLoS One. 2012;7(2):e31628. doi: 10.1371/journal.pone.0031628. Epub 2012 Feb 9.

Abstract

Runs of homozygosity (ROH) represents extended length of homozygotes on a long genomic distance. In oncology, it is known as loss of heterozygosity (LOH) if identified exclusively in cancer cell rather than in matched control cell. Studies have identified several genomic regions which show consistent ROH in different kinds of carcinoma. To query whether this consistency can be observed on broader spectrum, both in more cancer types and in wider genomic regions, we investigated ROH patterns in the National Cancer Institute 60 cancer cell line panel (NCI-60) and HapMap Caucasian healthy trio families. Using results from Affymetrix 500 K SNP arrays, we report a genome wide significant association of ROH regions between the NCI-60 and HapMap samples, with much a higher level of ROH (11 fold) in the cancer cell lines. Analysis shows that more severe ROH found in cancer cells appears to be the extension of existing ROH in healthy state. In the HapMap trios, the adult subgroup had a slightly but significantly higher level (1.02 fold) of ROH than did the young subgroup. For several ROH regions we observed the co-occurrence of fragile sites (FRAs). However, FRA on the genome wide level does not show a clear relationship with ROH regions.

摘要

纯合性运行(ROH)代表了在长基因组距离上的纯合子的延长长度。在肿瘤学中,如果仅在癌细胞中而不是在匹配的对照细胞中鉴定到,则其称为杂合性丢失(LOH)。研究已经确定了几个显示不同类型癌中一致 ROH 的基因组区域。为了查询这种一致性是否可以在更广泛的范围内观察到,包括更多种类的癌症和更广泛的基因组区域,我们研究了国家癌症研究所 60 种癌细胞系面板(NCI-60)和 HapMap 白种人健康三人组家庭中的 ROH 模式。使用 Affymetrix 500 K SNP 阵列的结果,我们报告了 NCI-60 和 HapMap 样本之间 ROH 区域的全基因组显著关联,癌细胞系中的 ROH 水平高得多(11 倍)。分析表明,在癌细胞中发现的更严重的 ROH 似乎是健康状态下现有 ROH 的延伸。在 HapMap 三人组中,成年亚组的 ROH 水平略高(1.02 倍),而年轻亚组则略高。对于几个 ROH 区域,我们观察到脆性位点(FRA)的共同发生。然而,基因组水平上的 FRA 与 ROH 区域没有明显的关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26dd/3276511/d8fee9901940/pone.0031628.g001.jpg

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