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30纳米染色质纤维可能结构的拓扑学限制

Topological constraints on the possible structures of the 30 nm chromatin fibre.

作者信息

Staynov D Z, Proykova Y G

机构信息

National Heart and Lung Institute, Imperial College London, Guy Scadding Building, Dovehouse St, London, SW3 6LY, UK.

出版信息

Chromosoma. 2008 Feb;117(1):67-76. doi: 10.1007/s00412-007-0127-3. Epub 2007 Oct 13.

Abstract

The packing of mammalian DNA into chromatin plays an important role in cell differentiation and selection of epigenetically marked genes for expression or silencing. The first level of folding, the nucleosome, is evolutionary conserved. It allows transcription, after remodeling and/or histone modifications. The second level, the transcriptionally dormant 30 nm fibre, exhibits species and tissue variations in the chromatin repeat length. Nevertheless, very similar structures of fibres have been observed in all metazoans, and therefore, have to accommodate variable linker lengths with a corresponding change of tilt of the nucleosomes, which is defined by the DNA helical periodicity. So far, none of the models for a regular fibre structure has considered this requirement nor the relationship between repeat length and orientations of nucleosomes in the fibre. Here, we present two regular structural arrangements with negatively tilted consecutive nucleosomes which can compensate for a non-integer number of bp/turn of DNA; one can accommodate a series of structures with discrete repeat lengths differing by 5 bp in the region around 200 bp and the other from around 220 to 250 bp, accommodating repeat lengths differing by 10 to 12 bp.

摘要

哺乳动物DNA包装成染色质在细胞分化以及选择进行表达或沉默的表观遗传标记基因方面发挥着重要作用。折叠的第一个层次,即核小体,在进化上是保守的。它在重塑和/或组蛋白修饰后允许转录。第二个层次,即转录休眠的30纳米纤维,在染色质重复长度上表现出物种和组织差异。然而,在所有后生动物中都观察到了非常相似的纤维结构,因此,必须通过核小体倾斜度的相应变化来适应可变的连接子长度,这是由DNA螺旋周期性定义的。到目前为止,没有一个规则纤维结构模型考虑到这一要求,也没有考虑重复长度与纤维中核小体取向之间的关系。在这里,我们提出了两种具有负倾斜连续核小体的规则结构排列,它们可以补偿非整数个DNA碱基对/转;一种可以容纳一系列结构,其在200 bp左右的区域内具有相差5 bp的离散重复长度,另一种在220至250 bp左右,容纳相差10至12 bp的重复长度。

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