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Suppression of initiation defects of chromosome replication in Bacillus subtilis dnaA and oriC-deleted mutants by integration of a plasmid replicon into the chromosomes.

机译:通过将质粒复制子整合到染色体中来抑制枯草芽孢杆菌dnaA和oriC缺失突变体中染色体复制的起始缺陷。

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摘要

We constructed Bacillus subtilis strains in which chromosome replication initiates from the minimal replicon of a plasmid isolated from Bacillus natto, independently of oriC. Integration of the replicon in either orientation at the proA locus (115 degrees on the genetic map) suppressed the temperature-sensitive phenotype caused by a mutation in dnaA, a gene required for initiation of replication from oriC. In addition, in a strain with the plasmid replicon integrated into the chromosome, we were able to delete sequences required for oriC function. These strains were viable but had a slower growth rate than the oriC+ strains. Marker frequency analysis revealed that both pyrD and metD, genes close to proA, showed the highest values among the markers (genes) measured, and those of other markers decreased symmetrically with distance from the site of the integration (proA). These results indicated that the integrated plasmid replicon operated as a new and sole origin of chromosome replication in these strains and that the mode of replication was bidirectional. Interestingly, these mutants produced anucleate cells at a high frequency (about 40% in exponential culture), and the distribution of chromosomes in the cells was irregular. A change in the site and mechanism (from oriC to a plasmid system) of initiation appears to have resulted in a drastic alteration in coordination between chromosome replication and chromosome partition or cell division.
机译:我们构建了枯草芽孢杆菌菌株,其中染色体复制从分离自纳豆芽孢杆菌的质粒的最小复制子开始,而与oriC无关。在proA基因座(遗传图谱上为115度)的任一方向复制子的整合抑制了由dnaA突变引起的温度敏感性表型,dnaA是从oriC启动复制所需的基因。此外,在将质粒复制子整合到染色体中的菌株中,我们能够删除oriC功能所需的序列。这些菌株是可行的,但生长速度比oriC +菌株慢。标记频率分析显示,与proA接近的pyrD和metD基因均在所测标记(基因)中显示出最高值,而其他标记的基因则随着距整合位点(proA)的距离对称地下降。这些结果表明,整合的质粒复制子在这些菌株中作为染色体复制的新的唯一来源,并且复制的模式是双向的。有趣的是,这些突变体以高频率产生无核细胞(在指数培养中约占40%),并且染色体在细胞中的分布是不规则的。起始位点和机制(从oriC到质粒系统)的变化似乎导致染色体复制与染色体分区或细胞分裂之间的配位发生了急剧变化。

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