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核小体与H1连接组蛋白相互作用的纳米尺度表征

Nanoscale Characterization of Interaction of Nucleosomes with H1 Linker Histone.

作者信息

Rafa Ahmed Yesvi, Filliaux Shaun, Lyubchenko Yuri L

机构信息

Department of Pharmaceutical Sciences, University of Nebraska Medical Center, Omaha, NE 68198-6025, USA.

出版信息

Int J Mol Sci. 2024 Dec 31;26(1):303. doi: 10.3390/ijms26010303.

Abstract

In eukaryotic nuclei, DNA is wrapped around an octamer of core histones to form nucleosomes. H1 binds to the linker DNA of nucleosome to form the chromatosome, the next structural unit of chromatin. Structural features on individual chromatosomes contribute to chromatin structure, but not fully characterized. In addition to canonical nucleosomes composed of two copies each of histones H2A, H2B, H3, and H4 (H3 nucleosomes), centromeres chromatin contain nucleosomes in which H3 is replaced with its analog CENP-A, changing structural properties of CENP-A nucleosomes. Nothing is known about the interaction of H1 with CENP-A nucleosomes. Here we filled this gap and characterized the interaction of H1 histone with both types of nucleosomes. H1 does bind both types of the nucleosomes forming more compact chromosome particles with elevated affinity to H3 nucleosomes. H1 binding significantly increases the stability of chromatosomes preventing their spontaneous dissociation. In addition to binding to the entry-exit position of the DNA arms identified earlier, H1 is capable of bridging of distant DNA segments. H1 binding leads to the assembly of mononucleosomes in aggregates, stabilized by internucleosome interactions as well as bridging of the DNA arms of chromatosomes. Contribution of these finding to the chromatin structure and functions are discussed.

摘要

在真核细胞核中,DNA缠绕在核心组蛋白八聚体周围形成核小体。H1与核小体的连接DNA结合形成染色质小体,这是染色质的下一个结构单元。单个染色质小体上的结构特征有助于染色质结构的形成,但尚未得到充分表征。除了由组蛋白H2A、H2B、H3和H4各两个拷贝组成的经典核小体(H3核小体)外,着丝粒染色质还包含核小体,其中H3被其类似物CENP-A取代,从而改变了CENP-A核小体的结构特性。关于H1与CENP-A核小体的相互作用尚不清楚。在这里,我们填补了这一空白,并表征了H1组蛋白与这两种类型核小体的相互作用。H1确实与这两种类型的核小体结合,形成了更紧密的染色体颗粒,对H3核小体具有更高的亲和力。H1的结合显著提高了染色质小体的稳定性,防止它们自发解离。除了与先前确定的DNA臂的进出位置结合外,H1还能够桥接远距离的DNA片段。H1的结合导致单核小体聚集成聚集体,通过核小体间相互作用以及染色质小体DNA臂的桥接而稳定。讨论了这些发现对染色质结构和功能的贡献。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5b25/11719560/2606d963d410/ijms-26-00303-g001.jpg

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