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多聚磷酸盐驱动细菌异染色质形成。

Polyphosphate drives bacterial heterochromatin formation.

作者信息

Beaufay Francois, Amemiya Haley M, Guan Jian, Basalla Joseph, Meinen Ben A, Chen Ziyuan, Mitra Rishav, Bardwell James C A, Biteen Julie S, Vecchiarelli Anthony G, Freddolino Lydia, Jakob Ursula

机构信息

Department of Molecular, Cellular and Developmental Biology, University of Michigan, Ann Arbor, MI, USA.

Cellular and Molecular Biology Program, Michigan Medicine, University of Michigan, Ann Arbor, MI, USA.

出版信息

Sci Adv. 2021 Dec 24;7(52):eabk0233. doi: 10.1126/sciadv.abk0233. Epub 2021 Dec 22.

Abstract

Heterochromatin is most often associated with eukaryotic organisms. Yet, bacteria also contain areas with densely protein-occupied chromatin that appear to silence gene expression. One nucleoid-associated silencing factor is the conserved protein Hfq. Although seemingly nonspecific in its DNA binding properties, Hfq is strongly enriched at AT-rich DNA regions, characteristic of prophages and mobile genetic elements. Here, we demonstrate that polyphosphate (polyP), an ancient and highly conserved polyanion, is essential for the site-specific DNA binding properties of Hfq in bacteria. Absence of polyP markedly alters the DNA binding profile of Hfq, causes unsolicited prophage and transposon mobilization, and increases mutagenesis rates and DNA damage–induced cell death. In vitro reconstitution of the system revealed that Hfq and polyP interact with AT-rich DNA sequences and form phase-separated condensates, a process that is mediated by the intrinsically disordered C-terminal extensions of Hfq. We propose that polyP serves as a newly identified driver of heterochromatin formation in bacteria.

摘要

异染色质通常与真核生物相关。然而,细菌也含有染色质被蛋白质密集占据的区域,这些区域似乎会使基因表达沉默。一种与核仁相关的沉默因子是保守蛋白Hfq。尽管Hfq在其DNA结合特性上看似非特异性,但它在富含AT的DNA区域高度富集,这是前噬菌体和移动遗传元件的特征。在这里,我们证明多聚磷酸盐(polyP),一种古老且高度保守的多阴离子,对于细菌中Hfq的位点特异性DNA结合特性至关重要。缺乏多聚磷酸盐会显著改变Hfq的DNA结合图谱,导致不必要的前噬菌体和转座子动员,并增加诱变率和DNA损伤诱导的细胞死亡。该系统的体外重建表明,Hfq和多聚磷酸盐与富含AT的DNA序列相互作用并形成相分离的凝聚物,这一过程由Hfq内在无序的C末端延伸介导。我们提出多聚磷酸盐是细菌中异染色质形成的新发现驱动因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5d45/10954037/2c244376d023/sciadv.abk0233-f1.jpg

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