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DnaA对pPS10宿主范围的调控

Modulation of pPS10 host range by DnaA.

作者信息

Maestro Beatriz, Sanz Jesús M, Faelen Michel, Couturier Martine, Díaz-Orejas Ramón, Fernández-Tresguerres Elena

机构信息

Departamento de Microbiología Molecular, Centro de Investigaciones Biológicas, Consejo Superior de Investigaciones Científicas, Madrid, Spain.

出版信息

Mol Microbiol. 2002 Oct;46(1):223-34. doi: 10.1046/j.1365-2958.2002.03155.x.

Abstract

Narrow-host-range plasmid pPS10, originally found in Pseudomonas savastanoi, is unable to replicate in other strains such as Escherichia coli. Here, we report that the establishment of pPS10 in E. coli can be achieved by a triple mutation in the dnaA gene of E. coli (dnaA403), leading to Q14amber, P297S and A412V changes in the DnaA host replication protein (DnaA403 mutant). As the E. coli strain used contained double amber suppressor mutations (supE, supF), the amber codon in dnaA403 can be translated into glutamine or tyrosine. Genetic analysis of DnaA proteins containing either the individual changes or their different combinations suggests that the P297S mutation is crucial for the establishment of the pPS10 replicon in E. coli. The data also indicate that the P297S change is toxic to the cell and that the additional mutations in DnaA403 could contribute to neutralize this toxicity. To our knowledge, this work reports the first chromosome mutant described in the literature that allows the host range broadening of a plasmid, highlights the essential role played by DnaA in the establishment of pPS10 replicon in E. coli and provides support for the hypothesis that interactions between RepA and DnaA modulate the establishment of pPS10 in that bacteria and probably in other species.

摘要

窄宿主范围质粒pPS10最初发现于野油菜黄单胞菌,无法在其他菌株如大肠杆菌中复制。在此,我们报道通过大肠杆菌dnaA基因的三重突变(dnaA403)可使pPS10在大肠杆菌中建立,该突变导致DnaA宿主复制蛋白发生Q14琥珀突变、P297S和A412V变化(DnaA403突变体)。由于所用的大肠杆菌菌株含有双重琥珀抑制突变(supE、supF),dnaA403中的琥珀密码子可被翻译成谷氨酰胺或酪氨酸。对含有单个变化或其不同组合的DnaA蛋白的遗传分析表明,P297S突变对于pPS10复制子在大肠杆菌中的建立至关重要。数据还表明,P297S变化对细胞有毒,而DnaA403中的其他突变可能有助于中和这种毒性。据我们所知,这项工作报道了文献中描述的第一个允许质粒宿主范围拓宽的染色体突变体,突出了DnaA在pPS10复制子于大肠杆菌中建立过程中所起的重要作用,并为RepA与DnaA之间的相互作用调节pPS10在该细菌以及可能在其他物种中的建立这一假说提供了支持。

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