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小鼠肝细胞核中大规模染色质结构的各个方面可以从DNA序列中预测出来。

Aspects of large-scale chromatin structures in mouse liver nuclei can be predicted from the DNA sequence.

作者信息

Cioffi Alfred, Fleury Tomara J, Stein Arnold

机构信息

Department of Biological Sciences, Purdue University, West Lafayette, IN 47907, USA.

出版信息

Nucleic Acids Res. 2006 Apr 13;34(7):1974-81. doi: 10.1093/nar/gkl078. Print 2006.

Abstract

The large amount of non-coding DNA present in mammalian genomes suggests that some of it may play a structural or functional role. We provide evidence that it is possible to predict computationally, from the DNA sequence, loci in mouse liver nuclei that possess distinctive nucleosome arrays. We tested the hypothesis that a 100 kb region of DNA possessing a strong, in-phase, dinucleosome period oscillation in the motif period-10 non-T, A/T, G, should generate a nucleosome array with a nucleosome repeat that is one-half of the dinucleosome oscillation period value, as computed by Fourier analysis of the sequence. Ten loci with short repeats, that would be readily distinguishable from the pervasive bulk repeat, were predicted computationally and then tested experimentally. We estimated experimentally that less than 20% of the chromatin in mouse liver nuclei has a nucleosome repeat length that is 15 bp, or more, shorter than the bulk repeat value of 195 +/- bp. All 10 computational predictions were confirmed experimentally with high statistical significance. Nucleosome repeats as short as 172 +/- 5 bp were observed for the first time in mouse liver chromatin. These findings may be useful for identifying distinctive chromatin structures computationally from the DNA sequence.

摘要

哺乳动物基因组中存在的大量非编码DNA表明,其中一些可能发挥结构或功能作用。我们提供的证据表明,从DNA序列通过计算预测小鼠肝细胞核中具有独特核小体阵列的位点是可能的。我们测试了这样一个假设:在基序周期为10的非T、A/T、G中具有强烈同相双核小体周期振荡的100 kb DNA区域,应产生一个核小体阵列,其核小体重复长度是通过对序列进行傅里叶分析计算出的双核小体振荡周期值的一半。通过计算预测了10个具有短重复序列的位点,这些位点很容易与普遍存在的大量重复序列区分开来,然后进行了实验验证。我们通过实验估计,小鼠肝细胞核中染色质的核小体重复长度比195 +/- bp的大量重复值短15 bp或更多的比例不到20%。所有10个计算预测都在实验中得到了高度统计学意义的证实。在小鼠肝染色质中首次观察到短至172 +/- 5 bp的核小体重复序列。这些发现可能有助于从DNA序列通过计算识别独特的染色质结构。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/33cf/1435979/5d0034a1aa97/gkl078f1.jpg

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