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Immunostaining of modified histones defines high-level features of the human metaphase epigenome.

机译:修饰组蛋白的免疫染色定义了人类中期表观基因组的高级特征。

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摘要

Immunolabeling of metaphase chromosome spreads can map components of the human epigenome at the single cell level. Previously, there has been no systematic attempt to explore the potential of this approach for epigenomic mapping and thereby to complement approaches based on chromatin immunoprecipitation (ChIP) and sequencing technologies. RESULTS: By immunostaining and immunofluorescence microscopy, we have defined the distribution of selected histone modifications across metaphase chromosomes from normal human lymphoblastoid cells and constructed immunostained karyotypes. Histone modifications H3K9ac, H3K27ac and H3K4me3 are all located in the same set of sharply defined immunofluorescent bands, corresponding to 10- to 50-Mb genomic segments.
机译:中期染色体扩散的免疫标记可以在单个细胞水平上绘制人类表观基因组的成分。以前,还没有系统的尝试来探索这种方法在表观基因组作图中的潜力,从而补充基于染色质免疫沉淀(ChIP)和测序技术的方法。结果:通过免疫染色和免疫荧光显微镜检查,我们确定了正常人淋巴母细胞在中期染色体上选择的组蛋白修饰的分布,并构建了免疫染色的核型。组蛋白修饰H3K9ac,H3K27ac和H3K4me3均位于同一组清晰定义的免疫荧光带中,对应于10至50 Mb的基因组片段。

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