Host inflammatory immune responses to oral microbiota are tightly regulated by multiple pro-inflammatory and anti-inflammatory mechanisms. The balance of there two activities ensures a state of immune homeostasis which is critical for protecting against microbial invasion and avoiding subsequent collateral tissue damages. To limit the ferocity of inflammation, a number of established pathways exist that dampen the innate immune response. Our recent publication has demonstrated a novel role for serum- and glucocorticoid- inducible kinase 1 (SGK1), a serine/threonine kinase associated with the PI3K pathway, in restraining the production of E. coil LPS-mediated pro-inflammatory cytokine production in human monocytes. Preliminary data for this application show for the first time that SGK1 is phospho-activated in human monocytes in response to challenge with multiple oral bacteria. In addition, using P. gingivalis, a well-established model oral organism for the investigation of host-pathogen interactions in the periodontium, we show that inhibition of SGK1 robustly enhances the production of pro-inflammatory cytokines (TNF, IL-12, IL-6, IL-1?, IL-8) and reduces IL-10 levels, a result also confirmed by using Cre-loxP-mediated SGK1 knockout mice. Moreover, the anti-inflammatory role for SGK1 was validated by our preliminary in vivo evidence showing that systemic administration of the SGK1 inhibitor, EMD638683, elevated infiltration of neutrophils and macrophages into the gingival tissues and aggravated the severity of alveolar bone resorption in mice orally infected with P. gingivalis. Thus, we have identified a novel role for SGK1 as a negative regulator of inflammation, and propose that stimulation of this endogenous anti-inflammatory pathway in the host will help limit or prevent P. gingivalis-induced tissue destruction. The specific hypothesis to be tested in this application is that in the context of P. gingivalis challenge, SGK1 constrains the production of pro-inflammatory cytokines; down-regulates recruitment of inflammatory cells to the periodontium; and in turn protects against alveolar bone loss through downstream modification of inflammatory signaling molecules including Nedd4-2, MKP-1, and TAK1, which ultimately converge on NF-?B. We will challenge this hypothesis with three specific Aims: (i) To characterize SGK1 as an innate immune suppressor of inflammatory responses in vitro; (ii) To elucidate the signaling mechanisms by which SGK1 controls host inflammatory responses; and (iii) To establish the in vivo relevance of SGK1 in the control of host inflammation using mouse subcutaneous chamber and alveolar bone loss models. Successful completion of these studies will characterize, for the first time, the anti-inflammatory function of SGK1 in host inflammatory responses to P. gingivalis, and elucidate the novel anti-inflammatory signaling network mediated by the SGK1-MKP1 module in the control of the inflammation progression. In the long term, this work could pave the way for the development of novel anti-inflammatory agents targeting SGK1 or MKP-1 to ameliorate or prevent not only P. gingivalis-induced tissue destruction, but other inflammatory disorders. Such an approach has relevance both for periodontal disease and for chronic inflammatory conditions in general.

Public Health Relevance

An uncontrolled host inflammatory immune response to a dysbiotic plaque community is the principal reason for the initiation and progression of multiple inflammatory diseases, including periodontal diseases such as chronic periodontitis. Thus, identification of the intracellular immune regulators that control the host response and elucidation of their related signaling networks are critical to redirect the dysregulated host inflammatory responses and develop the novel immunomodulatory therapeutic targets. We have identified a potent suppressor of the innate immune response to the classic bacterial agonist, LPS, called SGK1. In this study, we will characterize the role of SGK1 in the immune response to a representative oral pathogen with the ultimate goal of designing means to stimulate this molecule in order to constrain inflammatory destruction in gum disease.

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
7R01DE026727-03
Application #
9988663
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Chander, Preethi
Project Start
2019-08-21
Project End
2022-06-30
Budget Start
2019-08-21
Budget End
2020-06-30
Support Year
3
Fiscal Year
2019
Total Cost
Indirect Cost
Name
Virginia Commonwealth University
Department
Dentistry
Type
Schools of Dentistry/Oral Hygn
DUNS #
105300446
City
Richmond
State
VA
Country
United States
Zip Code
23298
Zhou, Wei; Su, Li; Duan, Xingyu et al. (2018) MicroRNA-21 down-regulates inflammation and inhibits periodontitis. Mol Immunol 101:608-614