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Hc1对DNA结构的介导作用:衣原体发育的潜在调节因子。

Hc1-mediated effects on DNA structure: a potential regulator of chlamydial development.

作者信息

Barry C E, Brickman T J, Hackstadt T

机构信息

Laboratory of Intracellular Parasites, NIAID, Rocky Mountain Laboratories, Hamilton, Montana 59840.

出版信息

Mol Microbiol. 1993 Jul;9(2):273-83. doi: 10.1111/j.1365-2958.1993.tb01689.x.

Abstract

Chlamydiae are obligate intracellular bacteria which undergo a unique developmental cycle, alternating between non-replicative elementary bodies (EBs) and replicative reticulate bodies (RBs). The transition from RB to EB is characterized by condensation of the chromosome into a dense nucleoid structure. The chlamydial histone homologue Hc1 is sufficient to induce formation of a similar structure in Escherichia coli. High-level Hc1 expression in E. coli is self-limiting and down-regulates transcription, translation, and replication at concentrations similar to those observed in chlamydial elementary bodies. Expression of Hc1 at sub-structural levels may have specific regulatory functions through its interaction with chromosomal DNA. In E. coli this is reflected in a dramatic shift in the pattern of gene expression. The differential expression of the outer membrane porin proteins OmpC and OmpF and analysis of lacZ fusions with promoter regions sensitive to supercoiling suggests that low-level Hc1 expression results in a net relaxation of chromosomal DNA. Topological analysis of plasmid DNA from both E. coli and Chlamydia trachomatis supports a decrease in superhelicity preceding nucleoid formation. In vitro analysis of purified Hc1-DNA interactions supports preferential binding based upon DNA conformation. These results suggest a dual role in which Hc1-mediated changes in gene expression may precede metabolic inactivity.

摘要

衣原体是专性细胞内细菌,经历独特的发育周期,在非复制性原体(EBs)和复制性网状体(RBs)之间交替。从RB到EB的转变特征是染色体浓缩成致密的类核结构。衣原体组蛋白同源物Hc1足以在大肠杆菌中诱导形成类似结构。大肠杆菌中Hc1的高水平表达是自我限制的,并且在与衣原体原体中观察到的浓度相似时下调转录、翻译和复制。亚结构水平的Hc1表达可能通过其与染色体DNA的相互作用具有特定的调节功能。在大肠杆菌中,这反映在基因表达模式的显著变化上。外膜孔蛋白OmpC和OmpF的差异表达以及与对超螺旋敏感的启动子区域的lacZ融合分析表明,低水平的Hc1表达导致染色体DNA的净松弛。来自大肠杆菌和沙眼衣原体的质粒DNA的拓扑分析支持在类核形成之前超螺旋度降低。纯化的Hc1-DNA相互作用的体外分析支持基于DNA构象的优先结合。这些结果表明Hc1介导的基因表达变化可能先于代谢不活跃的双重作用。

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