Oral Mucosal Endotoxin Tolerance Induction in Chronic Periodontitis

doi:10.1128/IAI.73.2.687-694.2005

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Infection and Immunity, February 2005, p. 687-694, Vol. 73, No. 2
0019-9567/05/$08.00+0 doi:10.1128/IAI.73.2.687-694.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

Oral Mucosal Endotoxin Tolerance Induction in Chronic Periodontitis

Manoj Muthukuru, Ravi Jotwani, and Christopher W. Cutler^*

Department of Periodontics, School of Dental Medicine, Stony Brook University—SUNY, Stony Brook, New York

Received 9 August 2004/ Returned for modification 3 October 2004/ Accepted 7 October 2004

The oral mucosa is exposed to a high density and diversity ofgram-positive and gram-negative bacteria, but very little isknown about how immune homeostasis is maintained in this environment,particularly in the inflammatory disease chronic periodontitis(CP). The cells of the innate immune response recognize bacterialstructures via the Toll-like receptors (TLR). This activatesintracellular signaling and transcription of proteins essentialfor the induction of an adaptive immune response; however, ifunregulated, it can lead to destructive inflammatory responses.Using single-immunoenzyme labeling, we show that the human oralmucosa (gingiva) is infiltrated by large numbers of TLR2⁺ andTLR4⁺ cells and that their numbers increase significantly inCP, relative to health (P < 0.05, Student's t test). We alsoshow that the numbers of TLR2⁺ but not TLR4⁺ cells increaselinearly with inflammation (r² = 0.33, P < 0.05). Double-immunofluorescenceanalysis confirms that TLR2 is coexpressed by monocytes (MC)/macrophages(m ${phi}$ ) in situ. Further analysis of gingival tissues by quantitativereal-time PCR, however, indicates that despite a threefold increasein the expression of interleukin-1ß (IL-1ß)mRNA during CP, there is significant (30-fold) downregulationof TLR2 mRNA (P < 0.05, Student's t test). Also showing similartrends are the levels of TLR4 (ninefold reduction), TLR5 (twofoldreduction), and MD-2 (sevenfold reduction) mRNA in CP patientscompared to healthy persons, while the level of CD14 was unchanged.In vitro studies with human MC indicate that MC respond to aninitial stimulus of lipopolysaccharide (LPS) from Porphyromonasgingivalis (PgLPS) or Escherichia coli (EcLPS) by upregulationof TLR2 and TLR4 mRNA and protein; moreover, IL-1ßmRNA is induced and tumor necrosis factor alpha (TNF- ${alpha}$ ), IL-10,IL-6, and IL-8 proteins are secreted. However, restimulationof MC with either PgLPS or EcLPS downregulates TLR2 and TLR4mRNA and protein and IL-1ß mRNA and induces a ca.10-fold reduction in TNF- ${alpha}$ secretion, suggesting the inductionof endotoxin tolerance by either LPS. Less susceptible to tolerancethan TNF- ${alpha}$ were IL-6, IL-10, and IL-8. These studies suggestthat certain components of the innate oral mucosal immune response,most notably TLRs and inflammatory cytokines, may become tolerizedduring sustained exposure to bacterial structures such as LPSand that this may be one mechanism used in the oral mucosa toattempt to regulate local immune responses.

* Corresponding author: Mailing address: Department of Periodontics, School of Dental Medicine, 110 Rockland Hall, Stony Brook University—SUNY, Stony Brook, NY 11794-8703. Phone: (631) 632-3025. Fax: (631) 631-3113. E-mail: Christopher.Cutler{at}stonybrook.edu.

Editor: J. D. Clements

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