Immune and regulatory functions of neutrophils in inflammatory bone loss

Summary A patient with leukocyte adhesion deficiency type 1 (LAD1) had severe periodontitis and an intractable, deep, nonhealing sacral wound. We had previously found a dominant interleukin-23–interleukin-17 signature at inflamed sites in humans with LAD1 and in mouse models of the disorder. Blockade of this pathway in mouse models has resulted in resolution of the immunopathologic condition. We treated our patient with ustekinumab, an antibody that binds the p40 subunit of interleukin-23 and interleukin-12 and thereby blocks the activity of these cytokines, inhibiting interleukin-23–dependent production of interleukin-17. After 1 year of therapy, our patient had resolution of his inflammatory lesions without serious infections or adverse reactions. Inhibition of interleukin-23 and interleukin-17 may have a role in the management of LAD1. (Funded by the National Institute of Allergy and Infectious Diseases and others.)

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“…2 Whether the immunopathologic consequences of tissue neutropenia in LAD1 are replicated in other forms of neutropenia remains to be seen.…”

Section: Discussionmentioning

confidence: 99%

“…1 The mucocutaneous lesions in LAD1 were widely assumed to be due to infections that were a result of the relative tissue neutropenia caused by the inability of LAD1 neutrophils to enter the tissue and control microbes. 2 However, recent work has shown that LAD1-associated oral disease is actually a microbe-induced hyperinflammatory response. 3,4 …”

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confidence: 99%

Interleukin-12 and Interleukin-23 Blockade in Leukocyte Adhesion Deficiency Type 1

Zerbe²,

et al. 2017

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“…Furthermore, congenital diseases, such as leukocyte adhesion deficiency, that impair neutrophil chemotaxis result in severe peri- odontitis at an early stage in life (46,47). In the mouse subcutaneous chamber model of infection, the newly appreciated periodontal pathogen F. alocis elicits a local inflammatory response with extensive neutrophil recruitment as well as spread to remote tissues, inducing lung edema with neutrophil recruitment and causing acute kidney injury (10).…”

Section: Discussionmentioning

confidence: 99%

Filifactor alocis Promotes Neutrophil Degranulation and Chemotactic Activity

et al. 2016

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Filifactor alocis is a recently recognized periodontal pathogen; however, little is known regarding its interactions with the immune system. As the first-responder phagocytic cells, neutrophils are recruited in large numbers to the periodontal pocket, where they play a crucial role in the innate defense of the periodontium. Thus, in order to colonize, successful periodontal pathogens must devise means to interfere with neutrophil chemotaxis and activation. In this study, we assessed major neutrophil functions, including degranulation and cell migration, associated with the p38 mitogen-activated protein kinase (MAPK) signaling pathway upon challenge with F. alocis. Under conditions lacking a chemotactic gradient, F. alocischallenged neutrophils had increased migration compared to uninfected cells, indicating that F. alocis increases chemokinesis in human neutrophils. In addition, neutrophil chemotaxis induced by interleukin-8 was significantly enhanced when cells were challenged with F. alocis, compared to noninfected cells. Similar to live bacteria, heat-killed F. alocis induced both random and directed migration of human neutrophils. The interaction of F. alocis with Toll-like receptor 2 induced granule exocytosis along with a transient ERK1/2 and sustained p38 MAPK activation. Moreover, F. alocis-induced secretory vesicle and specific granule exocytosis were p38 MAPK dependent. Blocking neutrophil degranulation with TAT-SNAP23 fusion protein significantly reduced the chemotactic and random migration induced by F. alocis. Therefore, we propose that induction of random migration by F. alocis will prolong neutrophil traffic time in the gingival tissue, and subsequent degranulation will contribute to tissue damage.

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“…CP does not result from individual pathogens but rather from polymicrobial synergy and dysbiosis (4) associated with a dysregulated immune response inducing inflammation-mediated tissue damage (5). Host genetic components have also been implicated in CP, with multiple genes contributing cumulatively to the host's overall disease risk (or protection) through effects on the host immune response and the microbiome (6). Since the Human Microbiome Project (HMP) (7), microbiota have been analyzed based on partial sequencing of the 16S rRNA gene, with different numbers of healthy and CP samples.…”

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confidence: 99%

Signature of Microbial Dysbiosis in Periodontitis

Meuric

Gall‐David

Boyer

et al. 2017

Appl Environ Microbiol

104

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Periodontitis is driven by disproportionate host inflammatory immune responses induced by an imbalance in the composition of oral bacteria; this instigates microbial dysbiosis, along with failed resolution of the chronic destructive inflammation. The objectives of this study were to identify microbial signatures for health and chronic periodontitis at the genus level and to propose a model of dysbiosis, including the calculation of bacterial ratios. Published sequencing data obtained from several different studies (196 subgingival samples from patients with chronic periodontitis and 422 subgingival samples from healthy subjects) were pooled and subjected to a new microbiota analysis using the same Visualization and Analysis of Microbial Population Structures (VAMPS) pipeline, to identify microbiota specific to health and disease. Microbiota were visualized using CoNet and Cytoscape. Dysbiosis ratios, defined as the percentage of genera associated with disease relative to the percentage of genera associated with health, were calculated to distinguish disease from health. Correlations between the proposed dysbiosis ratio and the periodontal pocket depth were tested with a different set of data obtained from a recent study, to confirm the relevance of the ratio as a potential indicator of dysbiosis. Beta diversity showed significant clustering of periodontitis-associated microbiota, at the genus level, according to the clinical status and independent of the methods used. Specific genera (Veillonella, Neisseria, Rothia, Corynebacterium, and Actinomyces) were highly prevalent (Ͼ95%) in health, while other genera (Eubacterium, Campylobacter, Treponema, and Tannerella) were associated with chronic periodontitis. The calculation of dysbiosis ratios based on the relative abundance of the genera found in health versus periodontitis was tested. Nonperiodontitis samples were significantly identifiable by low ratios, compared to chronic periodontitis samples. When applied to a subgingival sample set with well-defined clinical data, the method showed a strong correlation between the dysbiosis ratio, as well as a simplified ratio (Porphyromonas, Treponema, and Tannerella to Rothia and Corynebacterium), and pocket depth. Microbial analysis of chronic periodontitis can be correlated with the pocket depth through specific signatures for microbial dysbiosis.IMPORTANCE Defining microbiota typical of oral health or chronic periodontitis is difficult. The evaluation of periodontal disease is currently based on probing of the periodontal pocket. However, the status of pockets "on the mend" or sulci at risk of periodontitis cannot be addressed solely through pocket depth measurements or current microbiological tests available for practitioners. Thus, a more specific microbiological measure of dysbiosis could help in future diagnoses of periodontitis. In this work, data from different studies were pooled, to improve the accuracy of the results. However, analysis of multiple species from different studies intensified the bacteri...

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Immune and regulatory functions of neutrophils in inflammatory bone loss

Cited by 104 publications

References 219 publications

Interleukin-12 and Interleukin-23 Blockade in Leukocyte Adhesion Deficiency Type 1

Interleukin-12 and Interleukin-23 Blockade in Leukocyte Adhesion Deficiency Type 1

Filifactor alocis Promotes Neutrophil Degranulation and Chemotactic Activity

Signature of Microbial Dysbiosis in Periodontitis

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