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间期染色质动力学中的微尺度相干性。

Micron-scale coherence in interphase chromatin dynamics.

机构信息

Department of Systems Biology, Harvard Medical School, Boston, MA 02115.

出版信息

Proc Natl Acad Sci U S A. 2013 Sep 24;110(39):15555-60. doi: 10.1073/pnas.1220313110. Epub 2013 Sep 9.

Abstract

Chromatin structure and dynamics control all aspects of DNA biology yet are poorly understood, especially at large length scales. We developed an approach, displacement correlation spectroscopy based on time-resolved image correlation analysis, to map chromatin dynamics simultaneously across the whole nucleus in cultured human cells. This method revealed that chromatin movement was coherent across large regions (4-5 µm) for several seconds. Regions of coherent motion extended beyond the boundaries of single-chromosome territories, suggesting elastic coupling of motion over length scales much larger than those of genes. These large-scale, coupled motions were ATP dependent and unidirectional for several seconds, perhaps accounting for ATP-dependent directed movement of single genes. Perturbation of major nuclear ATPases such as DNA polymerase, RNA polymerase II, and topoisomerase II eliminated micron-scale coherence, while causing rapid, local movement to increase; i.e., local motions accelerated but became uncoupled from their neighbors. We observe similar trends in chromatin dynamics upon inducing a direct DNA damage; thus we hypothesize that this may be due to DNA damage responses that physically relax chromatin and block long-distance communication of forces.

摘要

染色质结构和动力学控制着 DNA 生物学的各个方面,但人们对此知之甚少,尤其是在大尺度上。我们开发了一种方法,即基于时间分辨图像相关分析的位移相关光谱学,以在培养的人类细胞中同时绘制整个细胞核内的染色质动力学图谱。该方法表明,染色质运动在数秒内可以在大区域(4-5 µm)内保持相干。相干运动的区域延伸超出单个染色体区域的边界,表明在比基因大得多的长度尺度上运动的弹性耦合。这些大规模的、耦合的运动依赖于 ATP 并持续数秒,这可能解释了单个基因的 ATP 依赖性定向运动。主要核 ATP 酶(如 DNA 聚合酶、RNA 聚合酶 II 和拓扑异构酶 II)的扰动消除了微米级的相干性,同时导致快速、局部运动增加;即,局部运动加速,但与相邻区域失去耦合。在诱导直接 DNA 损伤时,我们观察到染色质动力学的类似趋势;因此,我们假设这可能是由于 DNA 损伤反应使染色质物理松弛并阻止力的长距离传递。

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Micron-scale coherence in interphase chromatin dynamics.间期染色质动力学中的微尺度相干性。
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