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首页> 外文期刊>Journal of bacteriology >Modulation of pPS10 Host Range by Plasmid-Encoded RepA Initiator Protein
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Modulation of pPS10 Host Range by Plasmid-Encoded RepA Initiator Protein

机译:质粒编码的RepA起始蛋白对pPS10宿主范围的调节

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We report here the isolation and analysis of novel repA host range mutants of pPS10, a plasmid originally found in Pseudomonas savastanoi. Upon hydroxylamine treatment, five plasmid mutants were selected for their establishment in Escherichia coli at 37°C, a temperature at which the wild-type form cannot be established. The mutations were located in different functional regions of the plasmid RepA initiation protein, and the mutants differ in their stable maintenance, copy number, and ability to interact with sequences of the basic replicon. Four of them have broadened their host range, and one of them, unable to replicate in Pseudomonas, has therefore changed its host range. Moreover, the mutants also have increased their replication efficiency in strains other than E. coli such as Pseudomonas putida and Alcaligenes faecalis. None of these mutations drastically changed the structure or thermal stability of the wild-type RepA protein, but in all cases an enhanced interaction with host-encoded DnaA protein was detected by gel filtration chromatography. The effects of the mutations on the functionality of RepA protein are discussed in the framework of a three-dimensional model of the protein. We propose possible explanations for the host range effect of the different repA mutants, including the enhancement of limiting interactions of RepA with specific host replication factors such as DnaA.
机译:我们在这里报告了pPS10的新型 repA 宿主范围突变体的分离和分析,pPS10是最初在 Pseudomonas savastanoi 中发现的质粒。经羟胺处理后,选择了五个质粒突变体以在37°C(无法建立野生型的温度)下在大肠杆菌中建立。突变位于质粒RepA起始蛋白的不同功能区域,并且突变体在其稳定维持,拷贝数和与基本复制子序列相互作用的能力方面有所不同。其中四个扩大了寄主范围,其中一个无法在假单胞菌中复制,因此改变了其寄主范围。此外,这些突变体还提高了在除 E 以外的菌株中的复制效率。 大肠菌,例如 Pseudomonas putida 粪产碱菌。这些突变都没有彻底改变野生型RepA蛋白的结构或热稳定性,但在所有情况下,通过凝胶过滤色谱法检测到与宿主编码的DnaA蛋白的相互作用增强。在蛋白质三维模型的框架内讨论了突变对RepA蛋白功能的影响。我们提出了不同的 repA 突变体对宿主范围效应的可能解释,包括增强RepA与特定宿主复制因子(例如DnaA)的有限相互作用。

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