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Recombination phenotypes of the NCI-60 collection of human cancer cells

机译:NCI-60人类癌细胞集合的重组表型

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Background The NCI-60 is a collection of tumor cell lines derived from a variety of human adult cancer tissue types and is commonly used for genetic analysis and screening of potential chemotherapeutic agents. We wanted to understand the contributions of specific mechanisms of genomic instability to the etiology of cancers represented by the NCI-60.Results We screened the NCI-60 for dysregulated homologous recombination by using the gene cluster instability (GCI) assay we pioneered, and for defects in base excision repair by sensitivity to 5-hydroxymethyl-2'-deoxyuridine (hmdUrd). We identified subsets of the NCI-60 lines that either displayed the characteristic molecular signature of GCI or were sensitive to hmdUrd. With the exception of the NCI-H23 lung cancer line, these phenotypes were not found to overlap. None of the lines examined in either subset exhibited significant changes in the frequency of sister chromatid exchanges (SCE), neither did any of the lines in either subset exhibit microsatellite instability (MSI) indicative of defects in DNA mismatch repair.Conclusions Gene cluster instability, sensitivity to hmdUrd and sister chromatid exchange are mechanistically distinct phenomena. Genomic instability in the NCI-60 appears to involve only one mechanism of instability for each individual cell line.
机译:背景NCI-60是源自多种人类成年癌症组织类型的肿瘤细胞系的集合,通常用于遗传分析和筛选潜在的化学治疗剂。我们想了解基因组不稳定的特定机制对以NCI-60为代表的癌症的病因学的影响。结果我们使用我们率先开发的基因簇不稳定性(GCI)分析方法筛选了NCI-60同源重组异常的方法,并针对对5-羟甲基-2'-脱氧尿苷(hmdUrd)敏感的碱基切除修复中的缺陷。我们鉴定了NCI-60系的子集,这些子集显示GCI的特征性分子特征或对hmdUrd敏感。除NCI-H23肺癌系外,未发现这些表型重叠。在任一子集中检查的品系均未显示出姐妹染色单体交换(SCE)的频率发生显着变化,在任何子集中的任何品系均未表现出指示DNA错配修复缺陷的微卫星不稳定性(MSI)。对hmdUrd和姐妹染色单体交换的敏感性是机制上不同的现象。 NCI-60中的基因组不稳定性似乎仅涉及每种细胞系的一种不稳定性机制。

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