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首页> 外文期刊>Nucleic Acids Research >FANCD2 binding identifies conserved fragile sites at large transcribed genes in avian cells
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FANCD2 binding identifies conserved fragile sites at large transcribed genes in avian cells

机译:Fancd2结合识别禽细胞中大转录基因的保守脆弱位点

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Common Chromosomal Fragile Sites (CFSs) are specific genomic regions prone to form breaks on metaphase chromosomes in response to replication stress. Moreover, CFSs are mutational hotspots in cancer genomes, showing that the mutational mechanisms that operate at CFSs are highly active in cancer cells. Orthologs of human CFSs are found in a number of other mammals, but the extent of CFS conservation beyond the mammalian lineage is unclear. Characterization of CFSs from distantly related organisms can provide new insight into the biology underlying CFSs. Here, we have mapped CFSs in an avian cell line. We find that, overall the most significant CFSs coincide with extremely large conserved genes, from which very long transcripts are produced. However, no significant correlation between any sequence characteristics and CFSs is found. Moreover, we identified putative early replicating fragile sites (ERFSs), which is a distinct class of fragile sites and we developed a fluctuation analysis revealing high mutation rates at the CFS gene PARK2, with deletions as the most prevalent mutation. Finally, we show that avian homologs of the human CFS genes despite their fragility have resisted the general intron size reduction observed in birds suggesting that CFSs have a conserved biological function.
机译:常见的染色体易碎位点(CFSS)是响应于复制应力的特异性基因组区域容易发生在中期染色体上的破裂。此外,CFSS是癌症基因组中的突变热点,表明在CFSS在CFSS中操作的突变机制在癌细胞中具有高度活性。在许多其他哺乳动物中发现了人类CFS的直脑,但在哺乳动物血统之外的CFS保护程度尚不清楚。来自远处相关生物的CFSS的表征可以为生物学底层CFSS提供新的洞察力。在这里,我们在禽细胞系中映射了CFSS。我们发现,总体而言,最重要的CFSS与极大的保守基因一致,从中生产了很长的转录物。但是,发现任何序列特征和CFS之间没有显着相关性。此外,我们鉴定了推定的早期复制脆弱位点(ERFS),其是一种不同类别的脆弱位点,并且我们在CFS基因PARK2中显露出高突变率的波动分析,缺失是最普遍的突变。最后,我们表明,尽管它们脆弱的禽流性的人类CFS基因的禽类同源物抵抗了鸟类中观察到的一般内含子大小,表明CFSS具有保守的生物学功能。

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