Modification in the
 ppk
 Gene of
 Helicobacter
 pylori
 during Single and Multiple Experimental Murine Infections

Ayraud, Sarah; Janvier, Blandine; Salaün, Laurence; Fauchère, Jean-Louis

doi:10.1128/iai.71.4.1733-1739.2003

Cited by 16 publications

(9 citation statements)

References 48 publications

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“…Many bacterial species contain another enzyme, PPK2, that also synthesizes poly P (18,51), but no ppk2 gene homolog was found in H. pylori genomes (51). In studies complementary to ours, others had reported that the ppk1 gene of Hp141v, a mutant H. pylori strain selected for an ability to maintain chronic infection in mice for 1 year, contained a 102-bp deletion, and that ppk1 inactivation reduced this strain's vigor in mice (7,8). They also suggested that inactivation of ppk1 in the unrelated strain X47-2AL made the strain unable to colonize mice.…”

supporting

confidence: 48%

Diverse Phenotypes Resulting from Polyphosphate Kinase Gene ( ppk1 ) Inactivation in Different Strains of Helicobacter pylori

et al. 2005

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Connections among biochemical pathways should help buffer organisms against environmental stress and affect the pace and trajectory of genome evolution. To explore these ideas, we studied consequences of inactivating the gene for polyphosphate kinase 1 (ppk1) in strains of Helicobacter pylori, a genetically diverse gastric pathogen. The PPK1 enzyme catalyzes synthesis of inorganic polyphosphate (poly P), a reservoir of high-energy phosphate bonds with multiple roles. Prior analyses in less-fastidious microbes had implicated poly P in stress resistance, motility, and virulence. In our studies, ppk1 inactivation caused the expected near-complete absence of poly P (>250-fold decrease) but had phenotypic effects that differed markedly among unrelated strains: (i) poor initial growth on standard brain heart infusion agar (five of six strains tested); (ii) weakened colonization of mice (4 of 5 strains); (iii) reduced growth on Ham's F-12 agar, a nutritionally limiting medium (8 of 11 strains); (iv) heightened susceptibility to metronidazole (6 of 17 strains); and (v) decreased motility in soft agar (1 of 13 strains). Complementation tests confirmed that the lack of growth of one ⌬ppk1 strain on F-12 agar and the inability to colonize mice of another were each due to ppk1 inactivation. Thus, the importance of ppk1 to H. pylori differed among strains and the phenotypes monitored. We suggest that quantitative interactions, as seen here, are common among genes that affect metabolic pathways and that H. pylori's high genetic diversity makes it well suited for studies of such interactions, their underlying mechanisms, and their evolutionary consequences.Many biochemical pathways are connected, in that a given metabolite can be generated and/or consumed by any of several enzymes, and the flux along one pathway can be influenced by genetic, culture-related, or environmental factors that affect traffic along complementary or competing pathways (30, 38). The resulting complex networks of interaction constitute a major focus of the new discipline of systems biology (see, e.g., reference 24); may underlie many of the epistasis (gene-gene interaction), penetrance, and quantitative-trait phenomena that are of major importance in medical, agricultural, and evolutionary genetics (13, 31); and are likely to affect the specificity and vigor of infection and virulence of pathogens. Metabolic networks exhibit intriguing formal similarities to phenomena such as food webs in natural ecosystems, patterns of human interaction, and the routing of electricity in power grids (43).It is with this perspective that we have been studying how inactivation of the ppk1 gene, which encodes polyphosphate kinase, affects Helicobacter pylori

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confidence: 48%

Diverse Phenotypes Resulting from Polyphosphate Kinase Gene ( ppk1 ) Inactivation in Different Strains of Helicobacter pylori

et al. 2005

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“…and P. aeruginosa, and for colonization of certain strains of H. pylori (7,49,63,70). Chickens are a natural zoonotic reservoir for C. jejuni, and contamination of commercial broiler flocks is thought to account for the majority of human C. jejuni infections (47).…”

Section: Figmentioning

confidence: 99%

Polyphosphate Kinase 1 Is a Pathogenesis Determinant in Campylobacter jejuni

Allan²,

et al. 2007

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Campylobacter jejuni is the leading cause of bacterial gastroenteritis in the developed world. Despite its prevalence, relatively little is known about C. jejuni's precise pathogenesis mechanisms, particularly in comparison to other well-studied enteric organisms such as Escherichia coli and Salmonella spp. Altered expression of phosphate genes in a C. jejuni stringent response mutant, together with known correlations between the stringent response, polyphosphate (poly-P), and virulence in other bacteria, led us to investigate the role of poly-P in C. jejuni stress survival and pathogenesis. All sequenced C. jejuni strains harbor a conserved putative polyphosphate kinase 1 predicted to be principally responsible for poly-P synthesis. We generated a targeted ppk1 deletion mutant (⌬ppk1) in C. jejuni strain 81-176 and found that ⌬ppk1, as well as the ⌬spoT stringent response mutant, exhibited low levels of poly-P at all growth stages. In contrast, wild-type C. jejuni poly-P levels increased significantly as the bacteria transitioned from log to stationary phase. Phenotypic analyses revealed that the ⌬ppk1 mutant was defective for survival during osmotic shock and low-nutrient stress. However, certain phenotypes associated with ppk1 deletion in other bacteria (i.e., motility and oxidative stress) were unaffected in the C. jejuni ⌬ppk1 mutant, which also displayed an unexpected increase in biofilm formation. The C. jejuni ⌬ppk1 mutant was also defective for the virulence-associated phenotype of intraepithelial cell survival in a tissue culture infection model and exhibited a striking, dose-dependent chick colonization defect. These results indicate that poly-P utilization and accumulation contribute significantly to C. jejuni pathogenesis and affect its ability to adapt to specific stresses and stringencies. Furthermore, our study demonstrates that poly-P likely plays both similar and unique roles in C. jejuni compared to its roles in other bacteria and that poly-P metabolism is linked to stringent response mechanisms in C. jejuni.

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“…In mammals, polyP seems to play a role in blood coagulation [6][7][8]. In bacteria, polyP has chaperone-like activity [9], and regulates stress response, ion channels [10,11] and infectivity as demonstrated for Pseudomonas aeruginosa [10,11,12] and Helicobacter pylori [13]. In trypanosomes, polyP metabolism has been recently characterized and as in pathogenic bacteria, trypanosomes with reduced polyP levels are significantly less virulent [14].…”

Section: Introductionmentioning

confidence: 98%

The new world of inorganic polyphosphates

Azevedo

Saiardi

2016

Biochemical Society Transactions

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Post-translational modifications (PTMs) add regulatory features to proteins that help establish the complex functional networks that make up higher organisms. Advances in analytical detection methods have led to the identification of more than 200 types of PTMs. However, some modifications are unstable under the present detection methods, anticipating the existence of further modifications and a much more complex map of PTMs. An example is the recently discovered protein modification polyphosphorylation. Polyphosphorylation is mediated by inorganic polyphosphate (polyP) and represents the covalent attachment of this linear polymer of orthophosphate to lysine residues in target proteins. This modification has eluded MS analysis as both polyP itself and the phosphoramidate bonds created upon its reaction with lysine residues are highly unstable in acidic conditions. Polyphosphorylation detection was only possible through extensive biochemical characterization. Two targets have been identified: nuclear signal recognition 1 (Nsr1) and its interacting partner, topoisomerase 1 (Top1). Polyphosphorylation occurs within a conserved N-terminal polyacidic serine (S) and lysine (K) rich (PASK) cluster. It negatively regulates Nsr1-Top1 interaction and impairs Top1 enzymatic activity, namely relaxing supercoiled DNA. Modulation of cellular levels of polyP regulates Top1 activity by modifying its polyphosphorylation status. Here we discuss the significance of the recently identified new role of inorganic polyP.

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Modification in the ppk Gene of Helicobacter pylori during Single and Multiple Experimental Murine Infections

Cited by 16 publications

References 48 publications

Diverse Phenotypes Resulting from Polyphosphate Kinase Gene ( ppk1 ) Inactivation in Different Strains of Helicobacter pylori

Diverse Phenotypes Resulting from Polyphosphate Kinase Gene ( ppk1 ) Inactivation in Different Strains of Helicobacter pylori

Polyphosphate Kinase 1 Is a Pathogenesis Determinant in Campylobacter jejuni

The new world of inorganic polyphosphates

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