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用生物分子拥挤和交联蛋白 H-NS 对细菌染色体的压缩进行建模。

Modeling the compaction of bacterial chromosomes by biomolecular crowding and the cross-linking protein H-NS.

机构信息

Supercomputing Center, Korea Institute of Science and Technology Information, Daejeon, 34141, South Korea.

Department of Physics and Astronomy, University of Waterloo, Waterloo, ON, N2L 3G1, Canada.

出版信息

Sci Rep. 2024 Jan 2;14(1):139. doi: 10.1038/s41598-023-50355-2.

Abstract

Cells orchestrate the action of various molecules toward organizing their chromosomes. Using a coarse-grained computational model, we study the compaction of bacterial chromosomes by the cross-linking protein H-NS and cellular crowders. In this work, H-NS, modeled as a mobile "binder," can bind to a chromosome-like polymer with a characteristic binding energy. The simulation results reported here clarify the relative role of biomolecular crowding and H-NS in condensing a bacterial chromosome in a quantitative manner. In particular, they shed light on the nature and degree of crowder and H-NS synergetics: while the presence of crowders enhances H-NS binding to a chromosome-like polymer, the presence of H-NS makes crowding effects more efficient, suggesting two-way synergetics in chain compaction. Also, the results show how crowding effects promote clustering of bound H-NS. For a sufficiently large concentration of H-NS, the cluster size increases with the volume fraction of crowders.

摘要

细胞协调各种分子的作用,以组织它们的染色体。使用粗粒化计算模型,我们研究了交联蛋白 H-NS 和细胞拥挤对细菌染色体的压缩。在这项工作中,H-NS 被建模为一个可移动的“结合剂”,可以与具有特征结合能的染色体样聚合物结合。这里报道的模拟结果以定量的方式阐明了生物分子拥挤和 H-NS 在浓缩细菌染色体中的相对作用。特别是,它们揭示了拥挤和 H-NS 协同作用的性质和程度:虽然拥挤剂的存在增强了 H-NS 与染色体样聚合物的结合,但 H-NS 的存在使拥挤效应更有效,表明链压缩的双向协同作用。此外,结果还表明拥挤效应如何促进结合 H-NS 的聚类。对于足够大的 H-NS 浓度,簇的大小随拥挤剂的体积分数而增加。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c38c/10762067/f69b39fbc51f/41598_2023_50355_Fig1_HTML.jpg

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