Genome-wide fitness analyses of the foodborne pathogen Campylobacter jejuni in in vitro and in vivo models

Vries, Stefan P. W. de; Gupta, Shefali; Baig, Abiyad; Wright, Elli A.; Wedley, Amy; Jensen, Annette Nygaard; Lora, Lizeth LaCharme; Humphrey, Suzanne; Skovgård, Henrik; Macleod, Kareen; Pont, Elsa; Wolanska, Dominika P.; L’Heureux, Joanna; Mobegi, Fredrick M.; Smith, David George Emslie; Everest, Paul; Zomer, Aldert; Williams, Nicola; Wigley, Paul; Humphrey, T. J.; Maskell, Duncan J.; Grant, A.

doi:10.1038/s41598-017-01133-4

Cited by 45 publications

(60 citation statements)

References 88 publications

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“…Of the 98 mutations conferring increased in vitro fitness by DEseq2, validation experiments confirmed only 3 out of the 5 tested mutations (60%) ( Fig 2B ), revealing a slightly higher proportion of false-positive results with genes in this category. In general, false-positive results are not uncommon with Tn-seq screens [ 58 , 64 , 76 ] and may reflect a variety of reasons. The initial Tn-seq screen is a complex competitive environment involving thousands of mutants whereas validation studies tend to compare only a single mutant to the WT pathogen.…”

Section: Discussionmentioning

confidence: 99%

“…This result highlights that the 4 h in vitro library expansion step in our in vivo Tn-seq screen setting likely introduces some bias into our in vivo fitness datasets. Mutant pool expansion following in vivo Tn-seq screens, by mutant pool plating on agar [ 65 , 76 , 77 ] or culture in broth [ 64 , 78 ], is often required when library DNA extraction directly from tissue represents a limiting step to the Tn-seq procedure. This extra step is particularly important when using the Mme I-based Tn-seq approach [ 72 ], as it requires high quality DNA (no shearing).…”

Section: Discussionmentioning

confidence: 99%

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Genome-wide discovery of novel M1T1 group A streptococcal determinants important for fitness and virulence during soft-tissue infection

et al. 2017

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The Group A Streptococcus remains a significant human pathogen causing a wide array of disease ranging from self-limiting to life-threatening invasive infections. Epithelium (skin or throat) colonization with progression to the subepithelial tissues is the common step in all GAS infections. Here, we used transposon-sequencing (Tn-seq) to define the GAS 5448 genetic requirements for in vivo fitness in subepithelial tissue. A near-saturation transposon library of the M1T1 GAS 5448 strain was injected subcutaneously into mice, producing suppurative inflammation at 24 h that progressed to prominent abscesses with tissue necrosis at 48 h. The library composition was monitored en masse by Tn-seq and ratios of mutant abundance comparing the output (12, 24 and 48 h) versus input (T0) mutant pools were calculated for each gene. We identified a total of 273 subcutaneous fitness (scf) genes with 147 genes (55 of unknown function) critical for the M1T1 GAS 5448 fitness in vivo; and 126 genes (53 of unknown function) potentially linked to in vivo fitness advantage. Selected scf genes were validated in competitive subcutaneous infection with parental 5448. Two uncharacterized genes, scfA and scfB, encoding putative membrane-associated proteins and conserved among Gram-positive pathogens, were further characterized. Defined scfAB mutants in GAS were outcompeted by wild type 5448 in vivo, attenuated for lesion formation in the soft tissue infection model and dissemination to the bloodstream. We hypothesize that scfAB play an integral role in enhancing adaptation and fitness of GAS during localized skin infection, and potentially in propagation to other deeper host environments.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Genome-wide discovery of novel M1T1 group A streptococcal determinants important for fitness and virulence during soft-tissue infection

et al. 2017

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“…jejuni M1 adapts rapidly to introduction into a water environment, instigating gene expression changes that allow it to adapt to the stressful conditions, whilst maintaining viability. A recent complementary study by de Vries et al (2017) used Transposon Directed Insertion Sequencing (TRADIS) to identify genes essential for survival in vitro and in vivo [ 94 ]. Although comparing knockout studies to whole-transcriptome studies is difficult because gene knockouts will likely produce different transcriptional profiles due to deregulation or disruption of genetic pathways, in both studies a gene involved in the oxidative stress response: trxC , was identified as a key candidate gene for survival in model water systems.…”

Section: Discussionmentioning

confidence: 99%

Campylobacter jejuni transcriptome changes during loss of culturability in water

et al. 2017

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BackgroundWater serves as a potential reservoir for Campylobacter, the leading cause of bacterial gastroenteritis in humans. However, little is understood about the mechanisms underlying variations in survival characteristics between different strains of C. jejuni in natural environments, including water.ResultsWe identified three Campylobacter jejuni strains that exhibited variability in their ability to retain culturability after suspension in tap water at two different temperatures (4°C and 25°C). Of the three, strains C. jejuni M1 exhibited the most rapid loss of culturability whilst retaining viability. Using RNAseq transcriptomics, we characterised C. jejuni M1 gene expression in response to suspension in water by analyzing bacterial suspensions recovered immediately after introduction into water (Time 0), and from two sampling time/temperature combinations where considerable loss of culturability was evident, namely (i) after 24 h at 25°C, and (ii) after 72 h at 4°C. Transcript data were compared with a culture-grown control. Some gene expression characteristics were shared amongst the three populations recovered from water, with more genes being up-regulated than down. Many of the up-regulated genes were identified in the Time 0 sample, whereas the majority of down-regulated genes occurred in the 25°C (24 h) sample.ConclusionsVariations in expression were found amongst genes associated with oxygen tolerance, starvation and osmotic stress. However, we also found upregulation of flagellar assembly genes, accompanied by down-regulation of genes involved in chemotaxis. Our data also suggested a switch from secretion via the sec system to via the tat system, and that the quorum sensing gene luxS may be implicated in the survival of strain M1 in water. Variations in gene expression also occurred in accessory genome regions. Our data suggest that despite the loss of culturability, C. jejuni M1 remains viable and adapts via specific changes in gene expression.

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“…To assess the role of CapC in C. jejuni, isogenic mutants of capC were constructed in C. jejuni 81116 and C. jejuni M1 by insertion of a chloramphenicol resistance cassette. We were unable to complement the capC mutants, as we were unable to clone the capC coding sequence into the pC46 or pSV009 complementation vector in the correct orientation, despite repeated attempts (36)(37)(38).…”

Section: Resultsmentioning

confidence: 99%

CapC, a Novel Autotransporter and Virulence Factor of Campylobacter jejuni

Mehat

Park

Vliet

et al. 2018

Appl Environ Microbiol

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is recognized as an important causative agent of bacterial gastroenteritis in the developed world. Despite the identification of several factors contributing to infection, characterization of the virulence strategies employed by remains a significant challenge. Bacterial autotransporter proteins are a major class of secretory proteins in Gram-negative bacteria, and notably, many autotransporter proteins contribute to bacterial virulence. The aim of this study was to characterize the 81116 C8J_1278 gene (), predicted to encode an autotransporter protein, and examine the contribution of this factor to virulence of The predicted CapC protein has a number of features that are consistent with autotransporters, including the N-terminal signal sequence and the C-terminal β-barrel domain and was determined to localize to the outer membrane. Inactivation of the gene in 81116 and M1 resulted in reduced insecticidal activity in larvae. Furthermore, mutants displayed significantly reduced adherence to and invasion of nonpolarized, partially differentiated Caco-2 and T84 intestinal epithelial cells. Gentamicin treatment showed that the reduced invasion of the mutant is primarily caused by reduced adherence to intestinal epithelial cells, not by reduced invasion capability. mutants caused reduced interleukin 8 (IL-8) secretion from intestinal epithelial cells and elicited a significantly diminished immune reaction in larvae, indicating that CapC functions as an immunogen. In conclusion, CapC is a new virulence determinant of that contributes to the integral infection process of adhesion to human intestinal epithelial cells. is a major causative agent of human gastroenteritis, making this zoonotic pathogen of significant importance to human and veterinary public health worldwide. The mechanisms by which interacts with intestinal epithelial cells and causes disease are still poorly understood due, in part, to the heterogeneity of infection biology. Given the importance of to public health, the need to characterize novel and existing virulence mechanisms is apparent. The significance of our research is in demonstrating the role of CapC, a novel virulence factor in that contributes to adhesion and invasion of the intestinal epithelium, thereby in part, addressing the dearth of knowledge concerning the factors involved in pathogenesis and the variation observed in the severity of human infection.

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Genome-wide fitness analyses of the foodborne pathogen Campylobacter jejuni in in vitro and in vivo models

Cited by 45 publications

References 88 publications

Genome-wide discovery of novel M1T1 group A streptococcal determinants important for fitness and virulence during soft-tissue infection

Genome-wide discovery of novel M1T1 group A streptococcal determinants important for fitness and virulence during soft-tissue infection

Campylobacter jejuni transcriptome changes during loss of culturability in water

CapC, a Novel Autotransporter and Virulence Factor of Campylobacter jejuni

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