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循环细胞中印迹和核结构的维持。

Maintenance of imprinting and nuclear architecture in cycling cells.

作者信息

Teller Kathrin, Solovei Irina, Buiting Karin, Horsthemke Bernhard, Cremer Thomas

机构信息

Department of Biology II, Ludwig Maximilians University, Grosshadernerstrasse 2, 82152 Planegg-Martinsried, Germany.

出版信息

Proc Natl Acad Sci U S A. 2007 Sep 18;104(38):14970-5. doi: 10.1073/pnas.0704285104. Epub 2007 Sep 11.

Abstract

Dynamic gene repositioning has emerged as an additional level of epigenetic gene regulation. An early example was the report of a transient, spatial convergence (< or =2 microm) of oppositely imprinted regions ("kissing"), including the Angelman syndrome/Prader-Willi syndrome (AS/PWS) locus and the Beckwith-Wiedemann syndrome locus in human lymphocytes during late S phase. It was argued that kissing is required for maintaining opposite imprints in cycling cells. Employing 3D-FISH with a BAC contig covering the AS/PWS region, light optical, serial sectioning, and quantitative 3D-image analysis, we observed that both loci always retained a compact structure and did not form giant loops. Three-dimensional distances measured among various, homologous AS/PWS segments in 393 human lymphocytes, 132 human fibroblasts, and 129 lymphoblastoid cells from Gorilla gorilla revealed a wide range of distances at any stage of interphase and in G(0). At late S phase, 4% of nuclei showed distances < or =2 microm, 49% showed distances >6 microm, and 18% even showed distances >8 microm. A similar distance variability was found for Homo sapiens (HSA) 15 centromeres in a PWS patient with a deletion of the maternal AS/PWS locus and for the Beckwith-Wiedemann syndrome loci in human lymphocytes. A transient kiss during late S phase between loci widely separated at other stages of the cell cycle seems incompatible with known global constraints of chromatin movements in cycling cells. Further experiments suggest that the previously observed convergence of AS/PWS loci during late S phase was most likely a side effect of the convergence of nucleolus organizer region-bearing acrocentric human chromosomes, including HSA 15.

摘要

动态基因重定位已成为表观遗传基因调控的一个额外层面。一个早期的例子是关于在S期后期人类淋巴细胞中,包括天使综合征/普拉德-威利综合征(AS/PWS)位点和贝克威思-维德曼综合征位点在内的反向印记区域(“亲吻”)的短暂空间汇聚(≤2微米)的报道。有人认为,亲吻对于维持循环细胞中的反向印记是必需的。通过使用覆盖AS/PWS区域的BAC重叠群进行三维荧光原位杂交(3D-FISH)、光学显微镜、连续切片和定量三维图像分析,我们观察到两个位点始终保持紧凑结构,并未形成巨大环。在393个人类淋巴细胞、132个人类成纤维细胞和129个来自大猩猩的淋巴母细胞中,对各种同源AS/PWS片段之间测量的三维距离显示,在间期的任何阶段和G(0)期都有广泛的距离范围。在S期后期,4%的细胞核显示距离≤2微米,49%显示距离>6微米,甚至18%显示距离>8微米。在一名缺失母源AS/PWS位点的普拉德-威利综合征患者中,人类15号染色体着丝粒以及人类淋巴细胞中的贝克威思-维德曼综合征位点也发现了类似的距离变异性。在细胞周期其他阶段广泛分离的位点在S期后期的短暂亲吻似乎与循环细胞中染色质运动的已知全局限制不相容。进一步的实验表明,先前观察到的S期后期AS/PWS位点的汇聚很可能是携带核仁组织区的近端着丝粒人类染色体(包括人类15号染色体)汇聚的副作用。

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