Sulphite : cytochrome c oxidoreductase deficiency in Campylobacter jejuni reduces motility, host cell adherence and invasion

Tareen, Abdul Malik; Dasti, Javid Iqbal; Zautner, Andreas E.; Groß, Uwe; Lugert, Raimond

doi:10.1099/mic.0.045567-0

Cited by 18 publications

(16 citation statements)

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“…Additionally, the sulfite oxidase SorA controlled by Cj1000 is also required for an efficient infection of intestinal epithelial cells by C. jejuni (Tareen et al, 2011). In this study, we showed that the O 2 consumption in the presence of sulfite as electron donors is reduced in the cj1000 mutant compared to wild-type and complemented mutant.…”

Section: Resultssupporting

confidence: 48%

“…jejuni also possesses multiple systems to fuel the respiratory chains with electrons, being able to utilize succinate, malate, formate, D-lactate, hydrogen and NADP(H) as electron donors (Hoffman & Goodman, 1982;Parkhill et al, 2000;Sellars et al, 2002). The hydABC operon encodes the Ni/Fe hydrogenase that catalyses the reversible oxidation of hydrogen gas (H 2 ); sorA (cj0005c) encodes a molybdopterine oxidoreductase, which along with Cj0004c (SorB), is a sulfite/ cytochrome c oxidoreductase (SOR) involved in the transformation of sulfite into sulfate and the release of electrons (Myers & Kelly, 2005;Tareen et al, 2011). The downregulation of these genes in the cj1000 : : aph mutant indicates that Cj1000 activates directly or indirectly several pathways involved in electron generation for respiration.…”

Section: Energy Metabolismmentioning

confidence: 99%

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Inactivation of the LysR regulator Cj1000 of Campylobacter jejuni affects host colonization and respiration

Dufour

Flint

et al. 2013

Microbiology

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Section: Resultssupporting

confidence: 48%

Section: Energy Metabolismmentioning

confidence: 99%

Inactivation of the LysR regulator Cj1000 of Campylobacter jejuni affects host colonization and respiration

Dufour

Flint

et al. 2013

Microbiology

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“…As with colonization, work investigating fundamental aspects of C. jejuni physiology and stress survival has also revealed roles for these properties in invasion and/or intracellular survival. Examples of factors modulating both fundamental properties and affecting host cell interactions include SorA, a sulfite-cytochrome c oxidoreductase that allows C. jejuni to use sulfite as an electron donor (51,75); AspA and AspB catalyzing fumarate production (53); Cj0952c, which affects chemotaxis toward formic acid (74); PaqPQ, involved in amino acid uptake (42); FeoB, which is important for ferrous iron acquisition (52); and SodB, required for detoxification of reactive oxygen intermediates (53,60). Mutants in several global regulators modulating aspects of physiology and/or stress survival also exhibit invasion and/or intracellular survival defects.…”

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confidence: 99%

FdhTU-Modulated Formate Dehydrogenase Expression and Electron Donor Availability Enhance Recovery ofCampylobacter jejunifollowing Host Cell Infection

et al. 2012

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bCampylobacter jejuni is a food-borne bacterial pathogen that colonizes the intestinal tract and causes severe gastroenteritis. Interaction with host epithelial cells is thought to enhance severity of disease, and the ability of C. jejuni to modulate its metabolism in different in vivo and environmental niches contributes to its success as a pathogen. A C. jejuni operon comprising two genes that we designated fdhT (CJJ81176_1492) and fdhU (CJJ81176_1493) is conserved in many bacterial species. Deletion of fdhT or fdhU in C. jejuni resulted in apparent defects in adherence and/or invasion of Caco-2 epithelial cells when assessed by CFU enumeration on standard Mueller-Hinton agar. However, fluorescence microscopy indicated that each mutant invaded cells at wild-type levels, instead suggesting roles for FdhTU in either intracellular survival or postinvasion recovery. The loss of fdhU caused reduced mRNA levels of formate dehydrogenase (FDH) genes and a severe defect in FDH activity. Cell infection phenotypes of a mutant deleted for the FdhA subunit of FDH and an ⌬fdhU ⌬fdhA double mutant were similar to those of a ⌬fdhU mutant, which likewise suggested that FdhU and FdhA function in the same pathway. Cell infection assays followed by CFU enumeration on plates supplemented with sodium sulfite abolished the ⌬fdhU and ⌬fdhA mutant defects and resulted in significantly enhanced recovery of all strains, including wild type, at the invasion and intracellular survival time points. Collectively, our data indicate that FdhTU and FDH are required for optimal recovery following cell infection and suggest that C. jejuni alters its metabolic potential in the intracellular environment.

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“…The resulting PCR product with a length of 3752 bp comprised of the complete cloning vector pBluescript, the 413 5′-terminal nucleotides and the 378 3′-terminal nucleotides of cj0268c . After gel extraction of the PCR product using the QIAquick PCR Purification Kit (Qiagen), a phosphorylated blunt end kanamycin resistance cassette described previously [21] was ligated with the obtained PCR product using Quick Ligase (New England Biolabs) following the instructions of the manufacturer to obtain plasmid pBcj0268c-kanR.…”

Section: Methodsmentioning

confidence: 99%

“…In addition to these proteins described to be involved in the process of adherence, also lipooligosaccharides (LOS) are important for pathogen-host cell interactions given that C. jejuni strains deficient in genes involved in LOS metabolism ( wlaRG, wlaTB and wlaTC ) exhibited diminished adherence properties to chicken embryo fibroblasts [20]. Recently, our group generated a C. jejuni mutant deficient in sulphite:cytochrome c oxidoreductase (SOR) which exhibited a down-regulated transcription of genes involved legionaminic acid synthesis and possessed reduced adherence properties to Caco2 cells [21]. Finally, a recently identified C. jejuni type VI secretion system (T6SS) was shown to be involved in cell adhesion.…”

Section: Introductionmentioning

confidence: 99%

The Campylobacter jejuni Cj0268c Protein Is Required for Adhesion and Invasion In Vitro

et al. 2013

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Adherence of Campylobacter jejuni to its particular host cells is mediated by several pathogen proteins. We screened a transposon-based mutant library of C. jejuni in order to identify clones with an invasion deficient phenotype towards Caco2 cells and detected a mutant with the transposon insertion in gene cj0268c. In vitro characterization of a generated non-random mutant, the mutant complemented with an intact copy of cj0268c and parental strain NCTC 11168 confirmed the relevance of Cj0268c in the invasion process, in particular regarding adherence to host cells. Whereas Cj0268c does not impact autoagglutination or motility of C. jejuni, heterologous expression in E. coli strain DH5α enhanced the potential of the complemented E. coli strain to adhere to Caco2 cells significantly and, thus, indicates that Cj0268c does not need to interact with other C. jejuni proteins to develop its adherence-mediating phenotype. Flow cytometric measurements of E. coli expressing Cj0268c indicate a localization of the protein in the periplasmic space with no access of its C-terminus to the bacterial surface. Since a respective knockout mutant possesses clearly reduced resistance to Triton X-100 treatment, Cj0268c contributes to the stability of the bacterial cell wall. Finally, we could show that the presence of cj0268c seems to be ubiquitous in isolates of C. jejuni and does not correlate with specific clonal groups regarding pathogenicity or pathogen metabolism.

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Sulphite : cytochrome c oxidoreductase deficiency in Campylobacter jejuni reduces motility, host cell adherence and invasion

Cited by 18 publications

References 50 publications

Inactivation of the LysR regulator Cj1000 of Campylobacter jejuni affects host colonization and respiration

Inactivation of the LysR regulator Cj1000 of Campylobacter jejuni affects host colonization and respiration

FdhTU-Modulated Formate Dehydrogenase Expression and Electron Donor Availability Enhance Recovery ofCampylobacter jejunifollowing Host Cell Infection

The Campylobacter jejuni Cj0268c Protein Is Required for Adhesion and Invasion In Vitro

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