A dual role for P2X7 receptor during Porphyromonas gingivalis infection

Authors

E. S. Ramos-Junior, Universidade Federal do Rio de Janeiro
Ana Carolina Morandini, University of the PacificFollow
Cassio Almeida-da-Silva, University of the Pacific, School of DentistryFollow
E. J. Franco, Catholic University of Brasília
J. Potempa, University of Louisville
K. A. Nguyen, University of Sydney
A. C. Oliveira, Universidade Federal do Rio de Janeiro
D. S. Zamboni, University of São Paulo
David M. Ojcius, University of the PacificFollow
J. Scharfstein, Universidade Federal do Rio de Janeiro
Robson Coutinho-Silva, Universidade Federal do Rio de JaneiroFollow

ORCiD

David M. Ojcius: 0000-0003-1461-4495, Ana C. Morandini: 0000-0003-4749-571X

Department

Biomedical Sciences

Document Type

Article

Publication Title

Journal of Dental Research

ISSN

0022-0345

Volume

94

Issue

9

DOI

10.1177/0022034515593465

First Page

1233

Last Page

1242

Publication Date

1-1-2015

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.

Recommended Citation

Ramos-Junior, E. S., Morandini, A. C., Almeida-da-Silva, C., Franco, E. J., Potempa, J., Nguyen, K. A., Oliveira, A. C., Zamboni, D. S., Ojcius, D. M., Scharfstein, J., & Coutinho-Silva, R. (2015). A dual role for P2X7 receptor during Porphyromonas gingivalis infection. Journal of Dental Research, 94(9), 1233–1242. DOI: 10.1177/0022034515593465
https://scholarlycommons.pacific.edu/dugoni-facarticles/24