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人类端粒染色质的柱状结构。

Columnar structure of human telomeric chromatin.

作者信息

Soman Aghil, Wong Sook Yi, Korolev Nikolay, Surya Wahyu, Lattmann Simon, Vogirala Vinod K, Chen Qinming, Berezhnoy Nikolay V, van Noort John, Rhodes Daniela, Nordenskiöld Lars

机构信息

School of Biological Sciences, Nanyang Technological University, Singapore, Singapore.

Department of Emerging Infectious Diseases, Duke-NUS, Medical School, Singapore, Singapore.

出版信息

Nature. 2022 Sep;609(7929):1048-1055. doi: 10.1038/s41586-022-05236-5. Epub 2022 Sep 14.

Abstract

Telomeres, the ends of eukaryotic chromosomes, play pivotal parts in ageing and cancer and are targets of DNA damage and the DNA damage response. Little is known about the structure of telomeric chromatin at the molecular level. Here we used negative stain electron microscopy and single-molecule magnetic tweezers to characterize 3-kbp-long telomeric chromatin fibres. We also obtained the cryogenic electron microscopy structure of the condensed telomeric tetranucleosome and its dinucleosome unit. The structure displayed close stacking of nucleosomes with a columnar arrangement, and an unusually short nucleosome repeat  length that comprised about 132 bp DNA wound in a continuous superhelix around histone octamers. This columnar structure is primarily stabilized by the H2A carboxy-terminal and histone amino-terminal tails in a synergistic manner. The columnar conformation results in exposure of the DNA helix, which may make it susceptible to both DNA damage and the DNA damage response. The conformation also exists in an alternative open state, in which one nucleosome is unstacked and flipped out, which exposes the acidic patch of the histone surface. The structural features revealed in this work suggest mechanisms by which protein factors involved in telomere maintenance can access telomeric chromatin in its compact form.

摘要

端粒是真核生物染色体的末端,在衰老和癌症中起关键作用,并且是DNA损伤和DNA损伤反应的靶点。在分子水平上,人们对端粒染色质的结构知之甚少。在这里,我们使用负染色电子显微镜和单分子磁镊来表征3千碱基对长的端粒染色质纤维。我们还获得了浓缩的端粒四核小体及其双核小体单元的低温电子显微镜结构。该结构显示核小体紧密堆积,呈柱状排列,并且核小体重复长度异常短,约132个碱基对的DNA以连续超螺旋的形式缠绕在组蛋白八聚体周围。这种柱状结构主要由H2A羧基末端和组蛋白氨基末端尾巴协同稳定。柱状构象导致DNA螺旋暴露,这可能使其易受DNA损伤和DNA损伤反应的影响。这种构象还以另一种开放状态存在,其中一个核小体未堆积且翻转出来,从而暴露了组蛋白表面的酸性区域。这项工作揭示的结构特征表明了参与端粒维持的蛋白质因子能够以紧密形式接近端粒染色质的机制。

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