Your search keyword '"Campylobacter fetus pathogenicity"' showing total 10 results

1. Mechanisms underlying Campylobacter fetus pathogenesis in humans: surface-layer protein variation in relapsing infections.

Author

Tu ZC, Gaudreau C, and Blaser MJ

Subjects

Bacterial Typing Techniques, Gene Expression Profiling, Genotype, Humans, Phenotype, Recurrence, Bacterial Proteins genetics, Campylobacter Infections microbiology, Campylobacter fetus genetics, Campylobacter fetus pathogenicity, Membrane Glycoproteins genetics

Abstract

Campylobacter fetus causes gastrointestinal and systemic infections in humans. Although relapse is common despite antibiotic treatment, the mechanisms are not well understood. The surface-layer proteins (SLPs) of C. fetus, which are critical in virulence, undergo high-frequency phenotypic switching due to recombination of sap homologues, resulting in antigenic variation. To investigate the mechanisms involved in relapsing C. fetus infections, we compared SLP variation in 4 pairs of C. fetus strains that infect humans; initial and follow-up isolations were performed 20 days to 34 months apart. Of the 4 pairs of strains, 2 had antigenic variation, and another provided evidence for selection for SLP-positive populations. Southern hybridization indicated recombination underlying the SLP variation and up-regulation. The fourth pair had the same SLP antigenic profile and sap homologue hybridization pattern, which is consistent with latency of the original strain in a privileged locus. In total, these findings indicate that relapse may reflect at least 3 differing pathogenetic pathways.

Published

2005

2. Conservation and diversity of sap homologues and their organization among Campylobacter fetus isolates.

Author

Tu ZC, Hui J, and Blaser MJ

Subjects

Animals, Antigenic Variation, Antigens, Bacterial genetics, Bacterial Proteins immunology, Base Sequence, Campylobacter fetus immunology, Campylobacter fetus isolation & purification, Campylobacter fetus pathogenicity, Conserved Sequence, DNA, Bacterial genetics, Genes, Bacterial, Genetic Variation, Genomic Islands, Humans, Molecular Sequence Data, Phylogeny, Promoter Regions, Genetic, Species Specificity, Bacterial Proteins genetics, Campylobacter fetus genetics, Membrane Glycoproteins

Abstract

Campylobacter fetus surface layer proteins (SLPs), encoded by sapA homologues, are important in virulence. In wild-type C. fetus strain 23D, all eight sapA homologues are located in the 54-kb sap island, and SLP expression reflects the position of a unique sapA promoter in relation to the sapA homologues. The extensive homologies in the sap island include both direct and inverted repeats, which allow DNA rearrangements, deletion, or duplication; these elements confer substantial potential for genomic plasticity. To better understand C. fetus sap island diversity and variation mechanisms, we investigated the organization and distribution of sapA homologues among 18 C. fetus strains of different subspecies, serotypes, and origins. For all type A strains, the boundaries of the sap island were relatively consistent. A 187-bp noncoding DNA insertion near the upstream boundary of the sap island was found in two of three reptile strains studied. The sapA homologue profiles were strain specific, and six new sapA homologues were recognized. Several homologues from reptile strains are remarkably conserved in relation to their corresponding mammalian homologues. In total, the observed differences suggest that the sap island has evolved differing genotypes that are plastic, perhaps enabling colonization of varied niches, in addition to antigenic variation.

Published

2004

3. [Pathogenesis of Campylobacter fetus infection].

Author

Fujimoto S

Subjects

Animals, Campylobacter fetus genetics, Gene Expression Regulation, Bacterial genetics, Gene Rearrangement, Humans, Promoter Regions, Genetic, Virulence genetics, Bacterial Proteins, Campylobacter Infections microbiology, Campylobacter fetus pathogenicity, Membrane Glycoproteins genetics, Membrane Glycoproteins immunology, Membrane Glycoproteins physiology, Virulence Factors

Abstract

Campylobacter fetus subsp. fetus is a zoonotic pathogen and cause opportunistic systemic infection in human who either are pregnant or have an underlying illness. Crystalline surface layer (S-layer), an external structure on the outer membrane is the prime virulence factor of this organism. S-layer is responsible for resistance to both leukocyte phagocytosis and the bactericidal effects of human serum. Antigenic variation of C. fetus surface antigen during infection also help the organism to escape from host immune-system and it is due to variation in the expression of the S-layer proteins (SLPs). C. fetus has multiple SLP-encoding genes and control the expression with inversion of a DNA segment containing the SLP promoter and/or homologous recombination.

Published

2003

4. Campylobacter surface-layers (S-layers) and immune evasion.

Author

Thompson SA

Subjects

Antigens, Bacterial genetics, Antigens, Bacterial immunology, Bacterial Proteins genetics, Blood Bactericidal Activity, Campylobacter fetus genetics, Campylobacter fetus pathogenicity, Campylobacter rectus genetics, Campylobacter rectus pathogenicity, Chromosome Inversion, Complement C3 antagonists & inhibitors, Cytokines antagonists & inhibitors, Cytokines biosynthesis, DNA, Bacterial metabolism, Gene Expression Regulation, Bacterial, Humans, Membrane Glycoproteins genetics, Periodontal Diseases immunology, Phagocytosis, Virulence, Antigenic Variation genetics, Bacterial Proteins immunology, Campylobacter fetus immunology, Campylobacter rectus immunology, Inflammation Mediators antagonists & inhibitors, Membrane Glycoproteins immunology, Periodontal Diseases microbiology

Abstract

Many pathogenic bacteria have evolved mechanisms for evading host immune systems. One evasion mechanism is manifest by the surface layer (S-layer), a paracrystalline protein structure composed of S-layer proteins (SLPs). The S-layer, possessed by 2 Campylobacter species (C. fetus and C. rectus), is external to the bacterial outer membrane and can have multiple functions in immune avoidance. C. fetus is a pathogen of ungulates and immunocompromised humans, in whom it causes disseminated bloodstream disease. In C. fetus, the S-layer is required for dissemination and is involved in 2 mechanisms of evasion. First, the S-layer confers resistance to complement-mediated killing in non-immune serum by preventing the binding of complement factor C3b to the C. fetus cell surface. S-layer expressing C. fetus strains remain susceptible to complement-independent killing, utilizing opsonic antibodies directed against the S-layer. However, C. fetus has also evolved a mechanism for avoiding antibody-mediated killing by high-frequency antigenic variation of SLPs. Antigenic variation is accomplished by complex DNA inversion events involving a family of multiple SLP-encoding genes and a single SLP promoter. Inversion events result in the expression of antigenically variant S-layers, which require distinct antibody responses for killing. C. rectus is implicated in the pathogenesis of periodontal disease and also possesses an S-layer that appears to be involved in evading the human system. Although studied less extensively than its C. fetus counterpart, the C. rectus S-layer appears to confer resistance to complement-mediated killing and to cause the down-regulation of proinflammatory cytokines.

Published

2002

5. Roles of the surface layer proteins of Campylobacter fetus subsp. fetus in ovine abortion.

Author

Grogono-Thomas R, Dworkin J, Blaser MJ, and Newell DG

Subjects

Animals, Bacterial Proteins analysis, Campylobacter fetus chemistry, Female, Molecular Weight, Pregnancy, Rabbits, Rec A Recombinases analysis, Sheep, Abortion, Veterinary etiology, Bacterial Proteins physiology, Campylobacter fetus pathogenicity, Membrane Glycoproteins

Abstract

The role of the surface (S)-layer proteins of Campylobacter fetus subsp. fetus has been investigated using an ovine model of abortion. Wild-type strain 23D induced abortion in up to 90% of pregnant ewes challenged subcutaneously. Isolates recovered from both dams and fetuses expressed S-layer proteins with variable molecular masses. The spontaneous S-layer-negative variant, strain 23B, neither colonized nor caused abortions in pregnant ewes. A series of isogenic sapA and recA mutants, derived from 23D, also were investigated in this model. A mutant (501 [sapA recA(+)]) caused abortion in one of five challenged animals and was recovered from the placenta of a second animal. Another mutant (502 [sapA recA]) with no S-layer protein expression caused no colonization or abortions in challenged animals but caused abortion when administered intraplacentally. Mutants 600(2) and 600(4), both recA, had fixed expression of 97- and 127-kDa S-layer proteins, respectively. Two of the six animals challenged with mutant 600(4) were colonized, but there were no abortions. As expected, all five strains recovered expressed a 127-kDa S-layer protein. In contrast, mutant 600(2) was recovered from the placentas of all five challenged animals and caused abortion in two. Unexpectedly, one of the 16 isolates expressed a 127-kDa rather than a 97-kDa S-layer protein. Thus, these studies indicate that S-layer proteins appear essential for colonization and/or translocation to the placenta but are not required to mediate fetal injury and that S-layer variation may occur in a recA strain.

Published

2000

6. The Campylobacter fetus S layer is not essential for initial interaction with HEp-2 cells.

Author

Graham LL and MacDonald KL

Subjects

Campylobacter fetus growth & development, Campylobacter fetus physiology, Humans, Kinetics, Tumor Cells, Cultured, Bacterial Adhesion, Bacterial Outer Membrane Proteins physiology, Bacterial Proteins, Campylobacter fetus pathogenicity, Membrane Glycoproteins

Abstract

In vitro adherence assays were used to determine whether the S layer mediated interactions between Campylobacter fetus subsp. venerealis strains and HEp-2 cells. At multiplicity of infection ratios ranging from 0.1:1 through 100:1, quantitation of bacterial adherence by light microscopy revealed that S layer deficient isogenic C. fetus 809K and C. fetus 810K were not less efficient in their attachment to HEp-2 cells; either S layer deficient C. fetus strains interacted with HEp-2 cells in greater numbers than the corresponding wild-type parent strains 809 and 810 or there was no significant difference in adherence levels between wild-type and mutant strains. Adherence of C. fetus strains to HEp-2 cells increased most during the first 2 h of a 22-h incubation period with only a slight increase in C. fetus cell numbers occurring subsequent to 2 h. At each assay point throughout this 22-h time period, equivalent numbers of wild-type and S layer deficient C. fetus strains were observed associated with HEp-2 cells. Prior to 2 h, adherence levels of all C. fetus strains exceeded those of Escherichia coli AB264 and Salmonella typhimurium SL1344. And, unlike S. typhimurium, C. fetus did not undergo significant replication following initial adherence to HEp-2 cells. Campylobacter fetus did not adhere to HEp-2 cells in a localized or aggregative pattern but were randomly distributed over individual HEp-2 cells and at no time during the assay with C. fetus were changes in HEp-2 cell morphology apparent. These data suggest that the S layer is not essential for mediating initial interactions between C. fetus and HEp-2 cells.

Published

1998

7. Molecular mechanisms of Campylobacter fetus surface layer protein expression.

Author

Dworkin J and Blaser MJ

Subjects

Animals, Antigenic Variation, Bacterial Outer Membrane Proteins biosynthesis, Bacterial Outer Membrane Proteins immunology, Campylobacter fetus pathogenicity, Chromosome Inversion, Chromosomes, Bacterial, DNA, Bacterial, Gene Rearrangement, Promoter Regions, Genetic, Recombination, Genetic, Virulence, Bacterial Outer Membrane Proteins genetics, Bacterial Proteins, Campylobacter fetus genetics, Gene Expression, Membrane Glycoproteins

Abstract

Cells of the Gram-negative bacteria Campylobacter fetus are covered by monomolecular arrays of surface layer proteins (SLPs) critical for both persistence in their natural hosts and for virulence. For C. fetus cells, expression of SLPs essentially eliminates C3b binding and their antigenic variation thwarts host immunological defences. Each cell possesses multiple partially homologous and highly conserved SLP gene cassettes, tightly clustered in the genome, that encode SLPs of 97-149 kDa. These attach non-covalently via a conserved N-terminus to the cell wall lipopolysaccharide. Recent studies indicate that C. fetus reassorts a single promoter, controlling SLP expression, and one, or more, complete open reading frame strictly by DNA inversion, and that rearrangement is independent of the distance between sites of inversion. In contrast to previously reported programmed DNA inversion systems, inversion in C. fetus is recA-dependent. These rearrangements permit variation in protein expression from the family of SLP genes and suggest an expanding paradigm of programmed DNA rearrangements among microorganisms.

Published

1997

8. High-frequency S-layer protein variation in Campylobacter fetus revealed by sapA mutagenesis.

Author

Blaser MJ, Wang E, Tummuru MK, Washburn R, Fujimoto S, and Labigne A

Subjects

Animals, Antigenic Variation, Antigens, Bacterial genetics, Bacteremia etiology, Bacterial Proteins immunology, Bacterial Proteins isolation & purification, Blood Bactericidal Activity, Campylobacter fetus immunology, Campylobacter fetus pathogenicity, Chromosome Mapping, Complement System Proteins metabolism, Conjugation, Genetic, Escherichia coli genetics, Freeze Etching, Gene Expression, Genes, Bacterial, Genetic Vectors, In Vitro Techniques, Mice, Mutagenesis, Bacterial Proteins genetics, Campylobacter fetus genetics, Membrane Glycoproteins

Abstract

Campylobacter fetus utilizes paracrystalline surface (S-) layer proteins that confer complement resistance and that undergo antigenic variation to facilitate persistent mucosal colonization in ungulates. C. fetus possesses multiple homologues of sapA, each of which encode full-length S-layer proteins. Disruption of sapA by a gene targeting method (insertion of kanamycin (km) resistance) caused the loss of C. fetus cells bearing full-length S-layer proteins and their replacement by cells bearing a 50 kDa truncated protein that was not exported to the cell surface. After incubation of the mutants with serum, the survival rate was approximately 2 x 10(-2). Immunoblots of survivors showed that phenotypic reversion involving high-level production of full-length (98, 127 or 149 kDa) S-layer proteins had occurred. Revertants were serum resistant but caused approximately 10-fold less bacteraemia in orally challenged mice than did the wild-type strain. Southern hybridizations of the revertants showed rearrangement of sapA homologues and retention of the km marker. These results indicate that there exists high-frequency generation of C. fetus sapA antigenic variants, and that intracellular mechanisms acting at the level of DNA reciprocal recombination play key roles in this phenomenon.

Published

1994

9. Pathogenesis of Campylobacter fetus infections: critical role of high-molecular-weight S-layer proteins in virulence.

Author

Blaser MJ and Pei Z

Subjects

Animals, Antigens, Bacterial physiology, Blood Bactericidal Activity, Campylobacter Infections immunology, Campylobacter fetus immunology, Campylobacter fetus metabolism, Immunization, Passive, Luminescent Measurements, Mice, Phagocytosis, Pronase metabolism, Virulence, Bacterial Proteins immunology, Campylobacter Infections microbiology, Campylobacter fetus pathogenicity, Membrane Glycoproteins

Abstract

Wild-type Campylobacter fetus strains possess high-molecular-weight S-layer proteins (S+) and are highly resistant to serum-mediated killing and phagocytosis. Spontaneous mutant strains lacking these proteins (S-) are serum and phagocytosis sensitive and have reduced virulence in a mouse model. Intact S+ cells were treated with pronase, which made them S- although genotypically S+ and had essentially no effect on other cellular proteins or on viability. Treatment with pronase, but not buffer alone, rendered these cells serum and phagocytosis sensitive and reduced mouse virulence to the level observed for the S- mutant cells. In related studies, purified S-layer proteins diminished neutrophil chemoluminescent responses to a heterologous particulate antigen. Finally, passive administration of antiserum to the 97-kDa S-layer protein partially protected mice against lethal challenge with the S+ strain. These studies define the contribution of the S-layer proteins to C. fetus virulence.

Published

1993

10. Surface array protein of Campylobacter fetus. Cloning and gene structure.

Author

Blaser MJ and Gotschlich EC

Subjects

Amino Acid Sequence, Bacterial Outer Membrane Proteins isolation & purification, Base Sequence, Campylobacter fetus pathogenicity, Cloning, Molecular, Gene Library, Membrane Glycoproteins isolation & purification, Molecular Sequence Data, Molecular Weight, Protein Conformation, Recombinant Proteins isolation & purification, Restriction Mapping, Ribosomes metabolism, Sequence Homology, Nucleic Acid, Terminator Regions, Genetic, Virulence genetics, Bacterial Outer Membrane Proteins genetics, Bacterial Proteins, Campylobacter fetus genetics, Genes, Bacterial, Membrane Glycoproteins genetics, Membrane Proteins genetics

Abstract

The high molecular mass (97-149 kDa) surface array proteins (SAP) of Campylobacter fetus are critical to virulence. We created a bank of 160,000 random 1.0-6.5-kilobase (kb) chromosomal DNA fragments of C. fetus strain 84-32 (23D) using lambda gt11. Screening this bank in Escherichia coli Y1090 with antibody raised against purified SAP permitted isolation and purification of a clone with a 4.0-kb insert. Subcloning this insert in the E. coli vector, pUC9, permitted expression of a protein of approximately 100 kDa, not fused with beta-galactoside or inducible by isopropyl-beta-D-thiogalactopyranoside. Digestion with restriction endonucleases, and construction of deletion mutations indicated that the gene extended over 2.8 kb, proceeding toward the start of the beta-galactosidase gene. Taking advantage of a unique PstI site at 1.7 kb, we subcloned PstI-EcoRI fragments in both orientations into M13 vectors, then generated and sequenced 48 deletion mutants. In the 3974-base insert, an open reading frame, beginning at nucleotide 24 and terminating at 2825, was found to encode a 933-amino acid polypeptide having a calculated molecular mass of 96,758 daltons. The first 20 amino acids exactly match those determined from amino-terminal sequencing, indicating that this protein is secreted without a leader sequence. The deduced amino acid composition matches that of the purified SAP. We identified a ribosomal binding site 9 bases upstream, and a putative transcription terminator (delta G = -12.4) 21 bases downstream. There is partial homology of primary and secondary structure with five other bacterial S-layer proteins.

Published

1990