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A Contingency Locus in prfA in a Listeria monocytogenes Subgroup Allows Reactivation of the PrfA Virulence Regulator during Infection in Mice

机译:李斯特菌李斯特菌亚组中prfA的应急性位点允许在小鼠感染期间重新激活PrfA毒力调节剂。

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A nonhemolytic Listeria monocytogenes strain isolated from a fish processing plant was avirulent in a plaque-forming assay and in a subcutaneous mouse virulence assay. However, it showed 60% lethality (9/15 mice) when 10~(9) CFU were intraperitoneally injected into mice. Hemolytic L. monocytogenes bacteria were recovered from liver and spleen of the deceased mice, and the pulsed-field gel electrophoresis patterns were indistinguishable for the nonhemolytic and the hemolytic isolates. Sequencing of prfA from the nonhemolytic strain revealed a duplication of 7 bp in the helix-turn-helix region, resulting in a truncated PrfA protein. We propose that the direct repeat of 7 bp causes a reversible inactivation of prfA and that slipped-strand mispairing regulates the phase variation in hemolytic activity and virulence. Nonhemolytic L. monocytogenes strains with identical duplications in prfA were isolated from several sources in France, as well as in Norway, suggesting that the reversible inactivation described in this study is not an isolated event.
机译:从鱼加工厂分离出的非溶血性单核细胞增生李斯特菌菌株在噬菌斑形成试验和皮下小鼠毒性试验中无毒。然而,当腹膜内注射10〜(9)CFU时,它显示出60%的致死性(9/15小鼠)。从已故小鼠的肝脏和脾脏中回收了溶血性单核细胞增生李斯特菌,并且对于非溶血性和溶血性分离株,脉冲场凝胶电泳图谱是无法区分的。来自非溶血性菌株的prfA测序显示,螺旋-转-螺旋区重复7 bp,导致截短的PrfA蛋白。我们建议,直接重复7 bp导致prfA可逆失活,而滑链错配调节溶血活性和毒力的相变。从法国和挪威的几种来源中分离出在prfA中具有相同重复的非溶血性单核细胞增生李斯特菌菌株,这表明本研究中描述的可逆失活不是孤立事件。

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