Subversion of Innate Immunity by Periodontopathic Bacteria via Exploitation of Complement Receptor-3

Hajishengallis, George; Wang, Min; Liang, Shuang; Shakhatreh, Muhamad-Ali K.; James, Deanna; Nishiyama, So-ichiro; Yoshimura, Fuminobu; Demuth, Donald R.

doi:10.1007/978-0-387-78952-1_15

Cited by 38 publications

(39 citation statements)

References 64 publications

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“…Similarly, singlespecies infection using 10 7 CFU of P. gingivalis caused a small but not statistically significant increase in bone loss over shaminfected animals. Overall, these results are consistent with previous results from Baker et al (3) and our prior studies (17,37) that showed that infection using 10 9 CFU of P. gingivalis was required to induce significant levels of bone resorption. Interestingly, dual-species infection with 10 9 CFU of S. gordonii followed by 10 7 CFU of P. gingivalis induced significant bone loss, similar to that observed in the prior single infection experiments using 10 9 CFU of P. gingivalis (17,37).…”

Section: Discussionsupporting

confidence: 92%

Structural Dissection and In Vivo Effectiveness of a Peptide Inhibitor of Porphyromonas gingivalis Adherence to Streptococcus gordonii

et al. 2011

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The interaction of the minor fimbrial antigen (Mfa) with streptococcal antigen I/II (e.g., SspB) facilitates colonization of the dental biofilm by Porphyromonas gingivalis. We previously showed that a 27-mer peptide derived from SspB (designated BAR) resembles the nuclear receptor (NR) box protein-protein interacting domain and potently inhibits this interaction in vitro. Here, we show that the EXXP motif upstream of the NR core ␣-helix contributes to the Mfa-SspB interaction and that BAR reduces P. gingivalis colonization and alveolar bone loss in vivo in a murine model of periodontitis. Substitution of Gln for Pro 1171 or Glu 1168 increased the ␣-helicity of BAR and reduced its inhibitory activity in vitro by 10-fold and 2-fold, respectively. To determine if BAR prevents P. gingivalis infection in vivo, mice were first infected with Streptococcus gordonii and then challenged with P. gingivalis in the absence and presence of BAR. Animals that were infected with either 10 9 CFU of S. gordonii DL-1 or 10 7 CFU of P. gingivalis 33277 did not show a statistically significant increase in alveolar bone resorption over sham-infected controls. However, infection with 10 9 CFU of S. gordonii followed by 10 7 CFU of P. gingivalis induced significantly greater bone loss (P < 0.01) than sham infection or infection of mice with either organism alone. S. gordonii-infected mice that were subsequently challenged with 10 7 CFU of P. gingivalis in the presence of BAR exhibited levels of bone resorption similar to those of sham-infected animals. Together, these results indicate that both EXXP and the NR box are important for the Mfa-SspB interaction and that BAR peptide represents a potential therapeutic that may limit colonization of the oral cavity by P. gingivalis.Periodontal disease is an oral inflammatory disorder that is initiated by a microbial biofilm that forms in the subgingival pocket. In addition to the oral manifestation of periodontitis, periodontal pathogens such as Porphyromonas gingivalis are associated with a variety of other systemic disorders such as atherosclerosis, pneumonia, rheumatoid arthritis, and nephritis (7,10,12,23,24,26,28,29,34). However, colonization of the subgingival pocket by P. gingivalis can occur only after the organism first becomes established in the supragingival biofilm or on tissue surfaces. Colonization of the supragingival biofilm occurs through interspecies interactions of P. gingivalis with specific species of oral streptococci (e.g., Streptococcus oralis and Streptococcus gordonii but not the mutans streptococci) (11,20), and these initial interactions thus represent viable targets for therapeutic intervention to limit colonization of the oral cavity by P. gingivalis.The selective adherence of P. gingivalis to specific oral streptococcal species is driven by a protein-protein interaction that occurs between the minor fimbrial antigen (Mfa) of P. gingivalis and the streptococcal antigen I/II, and inactivation of mfa completely prevents P. gingivalis adherence and formation of biofil...

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Section: Discussionsupporting

confidence: 92%

Structural Dissection and In Vivo Effectiveness of a Peptide Inhibitor of Porphyromonas gingivalis Adherence to Streptococcus gordonii

et al. 2011

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“…There is no IgG or complement involved in PepO-induced phagocytosis by macrophages. Increasing evidence shows that CR3 is also a multifunctional pattern recognition receptor of the innate immune system (40)(41)(42)(43). Once activated by its ligand, CR3 mediates a series of signaling transductions, including rearrangement of actin, which promotes phagocytosis of bacteria by macrophages and contributes to the host defense response to bacterial infection.…”

Section: Discussionmentioning

confidence: 99%

Purified Streptococcus pneumoniae Endopeptidase O (PepO) Enhances Particle Uptake by Macrophages in a Toll-Like Receptor 2- and miR-155-Dependent Manner

et al. 2017

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Insights into the host-microbial virulence factor interaction, especially the immune signaling mechanisms, could provide novel prevention and treatment options for pneumococcal diseases. Streptococcus pneumoniae endopeptidase O (PepO) is a newly discovered and ubiquitously expressed pneumococcal virulence protein. A PepO-mutant strain showed impaired adherence to and invasion of host cells compared with the isogenic wild-type strain. It is still unknown whether PepO is involved in the host defense response to pneumococcal infection. Here, we demonstrated that PepO could enhance phagocytosis of Streptococcus pneumoniae and Staphylococcus aureus by peritoneal exudate macrophages (PEMs). Further studies showed that PepO stimulation upregulated the expression of microRNA-155 (miR-155) in PEMs in a time-and dose-dependent manner. PepO-induced enhanced phagocytosis was decreased in cells transfected with an inhibitor of miR-155, while it was increased in cells transfected with a mimic of miR-155. We also revealed that PepO-induced upregulation of miR-155 in PEMs was mediated by Toll-like receptor 2 (TLR2)-NF-B signaling and that the increased expression of miR-155 downregulated expression of SHIP1. Taken together, these results indicate that PepO induces upregulation of miR-155 in PEMs, contributing to enhanced phagocytosis and host defense response to pneumococci and Staphylococcus aureus.

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“…Thus, tight control of neutrophil functions and survival after bacterial clearance by induction of apoptosis, immune tolerance and resolution of inflammation, exert protective effects toward the host tissues against inflammatory tissue damage. A failure to properly regulate neutrophil abundance and turnover directly contributes to the pathogenesis of periodontitis and current literature implicates neutrophils as the main immune cell type responsible for periodontal disease progression (Hajishengallis et al, 2008b, 2015a; Scott and Krauss, 2012). …”

Section: Neutrophils In Periodontitismentioning

confidence: 99%

Manipulation of Neutrophils by Porphyromonas gingivalis in the Development of Periodontitis

Sochalska

Potempa

2017

Front. Cell. Infect. Microbiol.

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The pathogenesis of the chronic periodontal disease is associated with a skewed host inflammatory response to periodontal pathogens, such as Porphyromonas gingivalis, that accounts for the majority of periodontal tissue damage. Neutrophils are the most abundant leukocytes in periodontal pockets and depending on the stage of the disease, also plentiful PMNs are present in the inflamed gingival tissue and the gingival crevice. They are the most efficient phagocytes and eliminate pathogens by a variety of means, which are either oxygen-dependent or -independent. However, these secretory lethal weapons do not strictly discriminate between pathogens and host tissue. Current studies describe conflicting findings about neutrophil involvement in periodontal disease. On one hand literature indicate that hyper-reactive neutrophils are the main immune cell type responsible for this observed tissue damage and disease progression. Deregulation of neutrophil survival and functions, such as chemotaxis, migration, secretion of antimicrobial peptides or enzymes, and production of reactive oxygen species, contribute to observed tissue injury and the clinical signs of periodontal disease. On the other hand neutrophils deficiencies in patients and mice also result in periodontal phenotype. Therefore, P. gingivalis represents a periodontal pathogen that manipulates the immune responses of PMNs, employing several virulence factors, such as gingipains, serine proteases, lipid phosphatases, or fimbriae. This review will sum up studies devoted to understanding different strategies utilized by P. gingivalis to manipulate PMNs survival and functions in order to inhibit killing by a granular content, prolong inflammation, and gain access to nutrient resources.

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Subversion of Innate Immunity by Periodontopathic Bacteria via Exploitation of Complement Receptor-3

Cited by 38 publications

References 64 publications

Structural Dissection and In Vivo Effectiveness of a Peptide Inhibitor of Porphyromonas gingivalis Adherence to Streptococcus gordonii

Structural Dissection and In Vivo Effectiveness of a Peptide Inhibitor of Porphyromonas gingivalis Adherence to Streptococcus gordonii

Purified Streptococcus pneumoniae Endopeptidase O (PepO) Enhances Particle Uptake by Macrophages in a Toll-Like Receptor 2- and miR-155-Dependent Manner

Manipulation of Neutrophils by Porphyromonas gingivalis in the Development of Periodontitis

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