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The Cytolethal Distending Toxin Produced by Nontyphoidal Salmonella Serotypes Javiana, Montevideo, Oranienburg, and Mississippi Induces DNA Damage in a Manner Similar to That of Serotype Typhi

机译:非伤寒性沙门氏菌血清型Javiana,蒙得维的亚,奥拉宁堡和密西西比州产生的细胞致死性毒素诱导的DNA损伤类似于伤寒型的DNA

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ABSTRACT Select nontyphoidal Salmonella enterica (NTS) serotypes were recently found to encode the Salmonella cytolethal distending toxin (S-CDT), an important virulence factor for serotype Typhi, the causative agent of typhoid fever. Using a PCR-based assay, we determined that among 21 NTS serotypes causing the majority of food-borne salmonellosis cases in the United States, genes encoding S-CDT are conserved in isolates representing serotypes Javiana, Montevideo, and Oranienburg but that among serotype Mississippi isolates, the presence of S-CDT-encoding genes is clade associated. HeLa cells infected with representative strains of these S-CDT-positive serotypes had a significantly higher proportion of cells arrested in the G_(2)/M phase than HeLa cells infected with representative strains of S-CDT-negative serotypes Typhimurium, Newport, and Enteritidis. The G_(2)/M cell cycle arrest was dependent on CdtB, the active subunit of S-CDT, as infection with isogenic Δ cdtB mutants abolished their ability to induce a G_(2)/M cell cycle arrest. Infection with S-CDT-encoding serotypes was significantly associated with activation of the host cell’s DNA damage response (DDR), a signaling cascade that is important for detecting and repairing damaged DNA. HeLa cell populations infected with S-CDT-positive serotypes had a significantly higher proportion of cells with DDR protein 53BP1 and γH2AX foci than cells infected with either S-CDT-negative serotypes or isogenic Δ cdtB strains. Intoxication with S-CDT occurred via autocrine and paracrine pathways, as uninfected HeLa cells among populations of infected cells also had an activated DDR. Overall, we show that S-CDT plays a significant role in the cellular outcome of infection with NTS serotypes. IMPORTANCE The recent discovery that multiple serotypes encode S-CDT, which was previously established as an important virulence factor for serotype Typhi, suggested that this toxin may also contribute to the outcome of infection with nontyphoidal serotypes. In this study, we demonstrate that at a cellular level, S-CDT significantly alters the outcome of infection by inducing DNA damage which is associated with a cell cycle arrest and activation of the host cell’s DDR. Importantly, these results contribute valuable information for assessing the public health implications of S-CDT in infections with NTS serotypes. Our data suggest that infection with Salmonella strains that encode S-CDT has the potential to result in DNA damage, which may contribute to long-term sequelae.
机译:摘要最近发现,选择的非伤寒性肠炎沙门氏菌(NTS)血清型可编码沙门氏菌细胞致死性扩展毒素(S-CDT),这是伤寒型伤寒型Typhi血清型的重要毒力因子。使用基于PCR的分析,我们确定了在导致美国大多数食源性沙门氏菌病病例的21种NTS血清型中,编码S-CDT的基因在代表血清型Javiana,Montevideo和Oranienburg的分离株中是保守的,而在血清型密西西比州中在分离物中,编码S-CDT的基因的存在与进化枝相关。感染了这些S-CDT阳性血清型的代表性菌株的HeLa细胞比被感染S-CDT阴性血清型的鼠伤寒,纽波特,肠炎。 G_(2)/ M细胞周期阻滞依赖于S-CDT的活性亚基CdtB,因为等基因ΔcdtB突变体的感染消除了它们诱导G_(2)/ M细胞周期阻滞的能力。编码S-CDT的血清型感染与宿主细胞DNA损伤反应(DDR)的激活显着相关,DDR是一种信号级联,对于检测和修复受损的DNA非常重要。被S-CDT阳性血清型感染的HeLa细胞群体中具有DDR蛋白53BP1和γH2AX病灶的细胞比例明显高于被S-CDT阴性血清型或同基因ΔcdtB菌株感染的细胞。 S-CDT的中毒通过自分泌和旁分泌途径发生,因为感染细胞群体中未感染的HeLa细胞也具有激活的DDR。总体而言,我们显示S-CDT在感染NTS血清型的细胞结果中起重要作用。重要说明:最近发现多种血清型编码S-CDT(以前被确定为Tyty血清型的重要毒力因子)表明,该毒素也可能有助于非伤寒血清型的感染。在这项研究中,我们证明了在细胞水平上,S-CDT通过诱导DNA损伤显着改变感染的结果,DNA损伤与细胞周期停滞和宿主细胞DDR的激活有关。重要的是,这些结果为评估S-CDT在NTS血清型感染中对公共健康的影响提供了有价值的信息。我们的数据表明,编码S-CDT的沙门氏菌菌株感染可能导致DNA损伤,这可能会导致长期后遗症。

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