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首页> 外文期刊>Chromosome Research >Nucleosomal occupancy and CGG repeat expansion: a comparative analysis of triplet repeat region from mouse and human fragile X mental retardation gene 1
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Nucleosomal occupancy and CGG repeat expansion: a comparative analysis of triplet repeat region from mouse and human fragile X mental retardation gene 1

机译:核仁占用和CGG重复扩展:小鼠和人类脆弱的X智力低下基因1的三联体重复区域的比较分析

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The expansion of CGG repeats in the 5′-untranslated region (5′UTR) of FMR1 gene is the molecular basis of fragile X syndrome in most of the patients. The nature of the flanking sequences in addition to the length and interruption pattern of repeats is predicted to influence CGG repeat instability in the FMR1 gene. We investigated nucleosome occupancy as a contributor to CGG repeat instability in a transgenic mouse model containing unstable (CGG)26, from human FMR1 cloned downstream of nucleosome-excluding sequence. We observe that the transgene has an open chromatin structure compared to the stable endogenous mouse Fmr1 within the same nucleus. CGG repeats in mouse Fmr1 are flanked by nucleosomes unlike the repeats in the transgene in all the tissues examined. Further in vitro chromatin reconstitution experiments show that DNA fragment without the SV40ori/EPR (nucleosome-excluding sequence) forms more stable chromatin than the one containing it, despite having the same number of CGG repeats. The correlation between nucleosomal organisation of the FMR1 gene and CGG repeat instability was supported by significantly lower frequency of repeat expansion in mice containing an identical transgene without the SV40ori/EPR. Our studies demonstrate that flanking DNA sequences can influence repeat instability through modulation of nucleosome occupancy in the region.
机译:在大多数患者中,CMR重复序列在FMR1基因的5'-非翻译区(5'UTR)中的扩增是脆性X综合征的分子基础。预测除了重复序列的长度和中断模式外,侧翼序列的性质还会影响FMR1基因中CGG重复序列的不稳定性。我们调查了核小体的占用,这是在包含不稳定的(CGG) 26 的转基因小鼠模型中CGG重复不稳定性的原因,该模型来自克隆于核小体排除序列下游的人FMR1。我们观察到,与同一核内的稳定内源小鼠Fmr1相比,转基因具有开放的染色质结构。小鼠Fmr1中的CGG重复序列侧翼为核小体,这与所有检查的组织中转基因中的重复序列不同。进一步的体外染色质重建实验表明,尽管具有相同的CGG重复次数,但没有SV40ori / EPR(不包含核小体的序列)的DNA片段比包含其的DNA片段形成的染色质更稳定。 FMR1基因的核小体组织与CGG重复不稳定性之间的相关性由含有相同转基因但不含SV40ori / EPR的小鼠的重复扩增频率显着降低所支持。我们的研究表明,侧翼DNA序列可以通过调节该区域中核小体的占有率来影响重复的不稳定性。

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