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全球筛查和扩展命名 230 个依托泊苷诱导的脆性部位,包括 61 个尚未报道的脆性部位。

Global screening and extended nomenclature for 230 aphidicolin-inducible fragile sites, including 61 yet unreported ones.

机构信息

Institute of Human Genetics and Anthropology, D-07740 Jena, Germany.

出版信息

Int J Oncol. 2010 Apr;36(4):929-40. doi: 10.3892/ijo_00000572.

Abstract

Since the first description of human fragile sites (FS) more than 40 years ago, a variety of substances were reported to induce chromosomal breaks at non-random, breakage-prone regions. According to information available from human genome browsers aphidicolin, an inhibitor of DNA replication induces 77 of 88 known common FS. However, in the literature additional FS are reported, which are also, at least in part, inducible by aphidicolin. To the best of our knowledge, here we present the first and largest ever done systematic, whole genome-directed and comprehensive screening for aphidicolin-inducible breakage-prone regions. The study was performed on stimulated peripheral blood lymphocytes of 3 unrelated healthy individuals. Twenty-five thousand metaphase spreads were analyzed and overall 22,537 FS located in 230 different loci were recorded. Sixty-one of those FS were never observed before and 52 were already previously reported but not included in genome browsers and yet verified. Interestingly, aphidicolin was able to induce all types of rare and common FS, suggesting that these breakage-prone regions are less dependent on the inducing chemicals than originally supposed. Overall, we provide the first comprehensive genome wide map for FS and studied possible correlations of chromosome length and GTG-banding level with FS-frequency. To handle FS better in future, an extension of the already existing alphabetical nomenclature for FS on single chromosomes is suggested.

摘要

自 40 多年前首次描述人类脆弱部位(FS)以来,已有多种物质被报道可在非随机、易断裂的区域诱导染色体断裂。根据人类基因组浏览器提供的信息,DNA 复制抑制剂阿非迪可林可诱导 88 个已知常见 FS 中的 77 个。然而,文献中还报道了其他一些 FS,这些 FS 至少部分也可被阿非迪可林诱导。据我们所知,我们在这里首次进行了最大规模的、系统的、全基因组导向的和全面的阿非迪可林诱导易断裂部位筛选。该研究在 3 名无关健康个体的刺激外周血淋巴细胞中进行。分析了 25000 个中期分裂象,共记录了 230 个不同部位的 22537 个 FS。其中 61 个 FS 以前从未观察到过,52 个 FS 以前已经报道过,但未包含在基因组浏览器中,现在已经验证。有趣的是,阿非迪可林能够诱导所有类型的罕见和常见 FS,这表明这些易断裂部位比最初假设的对诱导化学物质的依赖性更小。总的来说,我们提供了第一个全面的 FS 全基因组图谱,并研究了染色体长度和 GTG 带型水平与 FS 频率之间的可能相关性。为了更好地处理未来的 FS,建议扩展现有的单个染色体 FS 字母命名法。

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