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Mapping in Vivo Chromatin Interactions in Yeast Suggests an Extended Chromatin Fiber with Regional Variation in Compaction*

机译:酵母中体内染色质相互作用的映射表明 扩展的染色质纤维具有区域差异 压实*

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摘要

The higher order arrangement of nucleosomes and the level of compaction of the chromatin fiber play important roles in the control of gene expression and other genomic activities. Analysis of chromatin in vitro has suggested that under near physiological conditions chromatin fibers can become highly compact and that the level of compaction can be modulated by histone modifications. However, less is known about the organization of chromatin fibers in living cells. Here, we combine chromosome conformation capture (3C) data with distance measurements and polymer modeling to determine the in vivo mass density of a transcriptionally active 95-kb GC-rich domain on chromosome III of the yeast Saccharomyces cerevisiae. In contrast to previous reports, we find that yeast does not form a compact fiber but that chromatin is extended with a mass per unit length that is consistent with a rather loose arrangement of nucleosomes. Analysis of 3C data from a neighboring AT-rich chromosomal domain indicates that chromatin in this domain is more compact, but that mass density is still well below that of a canonical 30 nm fiber. Our approach should be widely applicable to scale 3C data to real spatial dimensions, which will facilitate the quantification of the effects of chromatin modifications and transcription on chromatin fiber organization.
机译:核小体的高级排列和染色质纤维的紧密程度在控制基因表达和其他基因组活性中起着重要作用。体外染色质分析表明,在近乎生理条件下,染色质纤维可以变得高度紧密,并且紧密度水平可以通过组蛋白修饰来调节。然而,关于活细胞中染色质纤维的组织了解较少。在这里,我们将染色体构象捕获(3C)数据与距离测量和聚合物建模相结合,以确定酵母酿酒酵母III染色体上具有转录活性的95-kb富含GC的结构域的体内质量密度。与以前的报道相反,我们发现酵母不能形成紧密的纤维,但是染色质以每单位长度的质量扩展,这与核小体的相当宽松的排列相一致。对来自邻近富含AT的染色体结构域的3C数据的分析表明,该结构域中的染色质更紧密,但质量密度仍远低于规范的30 nm光纤。我们的方法应该广泛适用于将3C数据缩放到实际的空间尺寸,这将有助于量化染色质修饰和转录对染色质纤维组织的影响。

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    Dekker, Job;

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  • 年度 2008
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