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由Hfq的C末端结构域介导的DNA压缩与凝聚

Compaction and condensation of DNA mediated by the C-terminal domain of Hfq.

作者信息

Malabirade Antoine, Jiang Kai, Kubiak Krzysztof, Diaz-Mendoza Alvaro, Liu Fan, van Kan Jeroen A, Berret Jean-François, Arluison Véronique, van der Maarel Johan R C

机构信息

Laboratoire Léon Brillouin, CEA, CNRS, Université Paris Saclay, 91191 Gif-sur-Yvette, France.

Department of Physics, National University of Singapore, 2 Science Drive 3, 117542, Singapore.

出版信息

Nucleic Acids Res. 2017 Jul 7;45(12):7299-7308. doi: 10.1093/nar/gkx431.

Abstract

Hfq is a bacterial protein that is involved in several aspects of nucleic acids metabolism. It has been described as one of the nucleoid associated proteins shaping the bacterial chromosome, although it is better known to influence translation and turnover of cellular RNAs. Here, we explore the role of Escherichia coli Hfq's C-terminal domain in the compaction of double stranded DNA. Various experimental methodologies, including fluorescence microscopy imaging of single DNA molecules confined inside nanofluidic channels, atomic force microscopy, isothermal titration microcalorimetry and electrophoretic mobility assays have been used to follow the assembly of the C-terminal and N-terminal regions of Hfq on DNA. Results highlight the role of Hfq's C-terminal arms in DNA binding, change in mechanical properties of the double helix and compaction of DNA into a condensed form. The propensity for bridging and compaction of DNA by the C-terminal domain might be related to aggregation of bound protein and may have implications for protein binding related gene regulation.

摘要

Hfq是一种参与核酸代谢多个方面的细菌蛋白。它被描述为塑造细菌染色体的类核相关蛋白之一,尽管它因影响细胞RNA的翻译和周转而更为人所知。在这里,我们探讨了大肠杆菌Hfq的C端结构域在双链DNA压缩中的作用。我们使用了各种实验方法,包括对纳米流体通道内单个DNA分子的荧光显微镜成像、原子力显微镜、等温滴定量热法和电泳迁移率测定,来跟踪Hfq的C端和N端区域在DNA上的组装。结果突出了Hfq的C端臂在DNA结合、双螺旋机械性质变化以及DNA压缩成凝聚形式中的作用。C端结构域桥接和压缩DNA的倾向可能与结合蛋白的聚集有关,并且可能对与蛋白结合相关的基因调控有影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5f54/5499573/f9e0da15b1a3/gkx431fig1.jpg

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