Your search keyword '"Zamboni D"' showing total 4 results

1. NLRP12 Attenuates Inflammatory Bone Loss in Experimental Apical Periodontitis.

Author

Taira, T. M., Lima, V., Prado, D. S., Silva, T. A., Issa, J. P. M., da Silva, L. A. B., Zamboni, D. S., Cunha, F. Q., and Fukada, S. Y.

Subjects

PERIAPICAL periodontitis, BONE resorption, INFLAMMATION, PERIODONTAL disease, BIOLOGICAL tags, OSTEOCLASTS, DENTAL pulp diseases, ANIMAL experimentation, COMPARATIVE studies, COMPUTED tomography, MACROPHAGES, RESEARCH methodology, MEDICAL cooperation, MEMBRANE proteins, MICE, PERIAPICAL diseases, RESEARCH, EVALUATION research, SIGNAL peptides

Abstract

Apical periodontitis is an inflammatory disorder that results from the host immune response to microbial infection through the dental pulp, leading to alveolar bone destruction. The nod-like receptor 12 (NLRP12) is an atypical intracellular sensor of the NLR family that is involved in the negative regulation of several inflammatory conditions and also osteoclastogenesis. However, the role of NLRP12 in the regulation of immune response and bone loss induced by bacterial infection remains unclear. Here we investigated the development of apical periodontitis in wild-type (WT) and NLRP12 knockout (NLRP12-/-) mice by using micro-computed tomography together with histological, immunohistochemical, and molecular analyses. We found that NLRP12-/- mice are highly susceptible to apical periodontitis induced by bacterial infection, which is associated with an elevated infiltration of neutrophils and macrophages, periapical lesion extension, and alveolar bone destruction. Furthermore, NLRP12-/- mice showed a high expression of inflammatory cytokines ( Il1b, Il6, and Tnfa) and the osteoclastogenic markers ( Rankl and Acp5) in the periapical tissues. Consistent with this observation, NLRP12-/- mice showed an increased number of tartrate-resistant acid phosphatase-positive cells lining the apical periodontitis site, which was associated with augmented expression of the osteoclast effector genes, Ctsk and Mmp9. Mechanistically, NLRP12-deficient preosteoclasts showed elevated IκB-α degradation and p65 phosphorylation when stimulated with receptor activator of nuclear factor (NF)-κB ligand (RANKL). Similarly, increased IκB-α degradation was observed in the periapical tissue of NLRP12-/- mice. Furthermore, our in vitro study showed that preosteoclasts from NLRP12-/- mice exhibited higher RANKL-induced osteoclastogenesis, which was synergistically amplified by interleukin-1β and tumor necrosis factor α (mimicking an inflammatory periapical milieu). In conclusion, our data show that NLRP12 exhibits a protective role in the periapical bone destruction by attenuating inflammation and osteoclastogenesis through negative regulation of the NF-κB pathway. [ABSTRACT FROM AUTHOR]

Published

2019

2. A Dual Role for P2X7 Receptor during Porphyromonas gingivalis Infection.

Author

Ramos-Junior, E S, Morandini, A C, Almeida-da-Silva, C L C, Franco, E J, Potempa, J, Nguyen, K A, Oliveira, A C, Zamboni, D S, Ojcius, D M, Scharfstein, J, and Coutinho-Silva, R

Subjects

CELL receptors, ANIMALS, CARRIER proteins, GRAM-negative bacterial diseases, INTERLEUKIN-1, INTERLEUKINS, MICE, PROTEOLYTIC enzymes, TUMOR necrosis factors, GRAM-negative anaerobic bacteria, CELL physiology

Published

2015

3. A Dual Role for P2X7 Receptor during Porphyromonas gingivalis Infection.

Author

Ramos-Junior, E. S., Morandini, A. C., Almeida-da-Silva, C. L. C., Franco, E. J., Potempa, J., Nguyen, K. A., Oliveira, A. C., Zamboni, D. S., Ojcius, D. M., Scharfstein, J., and Coutinho-Silva, R.

Subjects

PORPHYROMONAS gingivalis infections, PURINERGIC receptors, CYTOKINES, INTERLEUKIN-1, INTERLEUKIN-18, PILI (Microbiology), MACROPHAGES, INTERLEUKIN-17

Abstract

Emerging evidence suggests a role for purinergic signaling in the activation of multiprotein intracellular complexes called inflammasomes, which control the release of potent inflammatory cytokines, such as interleukin (IL) -1β and -18. Porphyromonas gingivalis is intimately associated with periodontitis and is currently considered one of the pathogens that can subvert the immune system by limiting the activation of the NLRP3 inflammasome. We recently showed that P. gingivalis can dampen eATP-induced IL-1β secretion by means of its fimbriae in a purinergic P2X7 receptor–dependent manner. Here, we further explore the role of this purinergic receptor during eATP-induced IL-1β processing and secretion by P. gingivalis–infected macrophages. We found that NLRP3 was necessary for eATP-induced IL-1β secretion as well as for caspase 1 activation irrespective of P. gingivalis fimbriae. Additionally, although the secretion of IL-1β from P. gingivalis–infected macrophages was dependent on NLRP3, its adaptor protein ASC, or caspase 1, the cleavage of intracellular pro-IL-1β to the mature form was found to occur independently of NLRP3, its adaptor protein ASC, or caspase 1. Our in vitro findings revealed that P2X7 receptor has a dual role, being critical not only for eATP-induced IL-1β secretion but also for intracellular pro-IL-1β processing. These results were relevant in vivo since P2X7 receptor expression was upregulated in a P. gingivalis oral infection model, and reduced IFN-γ and IL-17 were detected in draining lymph node cells from P2rx7-/- mice. Furthermore, we demonstrated that P2X7 receptor and NLRP3 transcription were modulated in human chronic periodontitis. Overall, we conclude that the P2X7 receptor has a role in periodontal immunopathogenesis and suggest that targeting of the P2X7/NLRP3 pathway should be considered in future therapeutic interventions in periodontitis. [ABSTRACT FROM AUTHOR]

Published

2015

4. NOD2 contributes to Porphyromonas gingivalis-induced bone resorption.

Author

Prates, T P, Taira, T M, Holanda, M C, Bignardi, L A, Salvador, S L, Zamboni, D S, Cunha, F Q, and Fukada, S Y

Abstract

The NOD-like receptors are cytoplasmic proteins that sense microbial by-products released by invasive bacteria. Although NOD1 and NOD2 are functionally expressed in cells from oral tissues and play a role triggering immune responses, the role of NOD2 receptor in the bone resorption and in the modulation of osteoclastogenesis is still unclear. We show that in an experimental model of periodontitis with Porphyromonas gingivalis W83, NOD2(-/-) mice showed lower bone resorption when compared to wild type. Quantitative polymerase chain reaction analysis revealed that wild-type infected mice showed an elevated RANKL/OPG ratio when compared to NOD2(-/-) infected mice. Moreover, the expression of 2 osteoclast activity markers-cathepsin K and matrix metalloproteinase 9-was significantly lower in gingival tissue from NOD2(-/-) infected mice compared to WT infected ones. The in vitro study reported an increase in the expression of the NOD2 receptor 24 hr after stimulation of hematopoietic bone marrow cells with M-CSF and RANKL. We also evaluated the effect of direct activation of NOD2 receptor on osteoclastogenesis, by the activation of this receptor in preosteoclasts culture, with different concentrations of muramyl dipeptide. The results show no difference in the number of TRAP-positive cells. Although it did not alter the osteoclasts differentiation, the activation of NOD2 receptor led to a significant increase of cathepsin K expression. We confirm that this enzyme was active, since the osteoclasts resorption capacity was enhanced by muramyl dipeptide stimulation, evaluated in osteoassay plate. These results show that the lack of NOD2 receptor impairs the bone resorption, suggesting that NOD2 receptor could contribute to the progression of bone resorption in experimental model of periodontitis. The stimulation of NOD2 by its agonist, muramyl dipeptide, did not affect osteoclastogenesis, but it does favor the bone resorption capacity identified by increased osteoclast activity. [ABSTRACT FROM AUTHOR]

Published

2014