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首页> 外文期刊>Plasmid: An International Journal Devoted to Extrachromosomal Gene Systems >Conjugative and replicative biology of the Staphylococcus aureus antimicrobial resistance plasmid, pC02
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Conjugative and replicative biology of the Staphylococcus aureus antimicrobial resistance plasmid, pC02

机译:金黄色葡萄球菌抗菌抗性质粒的共轭和复制生物学,PC02

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Genetic transfer among bacteria propels rapid resistance to antibiotics and decreased susceptibility to antiseptics. Staphylococcus aureus is a common culprit of hospital and community acquired infections, and S. aureus plasmids have been shown to carry a multitude of antimicrobial resistance genes. We previously identified a novel conjugative, multidrug resistance plasmid, pC02, from the clinical S. aureus isolate C02. This plasmid contained the chlorhexidine resistance gene qacA, and we were able to demonstrate that conjugative transfer of pC02 imparted decreased chlorhexidine susceptibility to recipient strains. In silico sequence analysis of pC02 suggested that the plasmid is part of the pWBG749-family of conjugative plasmids and that it contains three predicted origins of transfer (oriT), two of which we showed were functional and could mediate plasmid transfer. Furthermore, depending on which oriT was utilized, partial transfer of pC02 was consistently observed. To define the ability of the pC02 plasmid to utilize different oriT sequences, we examined the mobilization ability of nonconjugative plasmid variants that were engineered to contain a variety of oriT family inserts. The oriT-OTUNa family was transferred at the highest frequency; additional oriT families were also transferred but at lower frequencies. Plasmid stability was examined, and the copy number of pC02 was defined using droplet digital PCR (ddPCR). pC02 was stably maintained at approximately 4 copies per cell. Given the conjugative plasticity of pC02, we speculate that this plasmid could contribute to the spread of antimicrobial resistance across Staphylococcal strains and species.
机译:细菌之间的遗传转移推动了抗生素的快速抵抗力,并降低了对抗疫苗的易感性。金黄色葡萄球菌是医院和群落获得的感染的共同罪魁祸首,并且已显示S.UUREUS质粒携带多种抗微生物抗性基因。我们以前鉴定了一种新的共轭,多药抗性质粒PC02,来自临床的金黄色葡萄球菌分离物CO 2。该质粒含有氯己定抗性基因Qaca,我们能够证明PC02的共轭转移赋予受体菌株的氯己定易感性降低。 PC02的硅序列分析表明,质粒是PWBG749的一部分 - 缀合质粒的一部分,其含有三个预测的转移起源(ORIT),其中两种转移(ORIT),我们显示出的两个是功能性的,并且可以介导质粒转移。此外,取决于利用的orit,始终观察到PC02的部分转移。为了定义PC02质粒利用不同的ORIT序列的能力,我们研究了非协定的质粒变体的动员能力,该变体被设计成含有各种矿石的家族插入物。 ORIT-OTUNA系列以最高频率转移;额外的orit家庭也被转移,但在较低的频率下。检查质粒稳定性,使用液滴数量PCR(DDPCR)定义PC02的拷贝数。 PC02每种细胞约4份稳定维持。鉴于PC02的共轭可塑性,我们推测该质粒可能有助于葡萄球菌菌株和物种的抗微生物抗性的扩散。

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