Periodontitis fuels the inflammation of obesity-associated type 2 diabetes (T2D), associates with poor glycemic control, and increases T2D morbidity. New strategies are critically needed to counter sources of periodontal infection and the resulting inflammation, both of which are refractory to standard treatments in people with T2D. However, mechanisms underlying the relationship between periodontitis and T2D remain poorly understood, impeding clinical progress. One unifying link between periodontitis and T2D is altered B cell function, and recent collaborative work between Drs. Barbara Nikolajczyk and Thomas Van Dyke showed that T2D-associated changes in B cells promote periodontitis. Our work further indicates that T cells cannot drive chronic periodontitis in T2D hosts in the absence of B cells, despite evidence that T cells promote periodontitis in lean hosts. Taken together, these findings support a model in which B cells support T2D-potentiated periodontitis, while T cells dominate periodontitis in leans. Both B cells and T cells are major sources of receptor activator of nuclear factor kappa-B ligand (RANKL), a key driver of osteoclastogenesis and periodontal bone loss. Obesity/T2D increases hematopoietic cell production of RANKL, most likely through increasing concentrations of a number of cytokines (TNF?, IL-1? and IL-6) known to drive RANKL production. These data, together with our demonstration that B cells are required for T2D-potentiated osteoclastogenesis and periodontitis, support our central hypothesis: T2D cytokines specifically up regulate B cell RANKL function, which uniquely potentiates periodontal complications of T2D. Definitive analyses are needed to fill the critical gaps in knowledge of how obesity-associated T2D impacts lymphocyte RANKL induction and function, and whether cellular sources of osteoclastogenic RANKL differ in T2D compared to lean hosts. We will use loss- and gain-of-function approaches in a standard mouse model of T2D, coupled with a standard model of chronic periodontitis, to study development of T2D-potentiated periodontal disease. We will complement the disease etiology work in mice with analysis of gingiva from people with T2D to query mechanistic underpinnings of chronic periodontitis. This strategy will identify drivers of both early and chronic phases of T2D-potentiated periodontitis to meet our long-term objective: to identify key factors that promote periodontitis in T2D compared to non-T2D subjects, and thereby pinpoint drug targets for future studies.

Public Health Relevance

Our proposed work will identify mechanisms by which lymphocytes (B cells and T cells) promote the pathogenic relationship between type 2 diabetes and periodontal disease. Identifying lymphocyte RANKL as a key mediator of type 2 diabetes-potentiated periodontal disease will pave the way for a greater understanding of disease pathogenesis, and raise the possibility that FDA-approved immunomodulatory drugs that are being tested as treatments for type 2 diabetes may positively impact periodontal complications.

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
5R01DE025383-02
Application #
9297280
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Chander, Preethi
Project Start
2016-07-01
Project End
2017-09-30
Budget Start
2017-07-01
Budget End
2017-09-30
Support Year
2
Fiscal Year
2017
Total Cost
Indirect Cost
Name
Boston University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
604483045
City
Boston
State
MA
Country
United States
Zip Code
02118
Mizraji, Gabriel; Heyman, Oded; Van Dyke, Thomas E et al. (2018) Resolvin D2 Restrains Th1 Immunity and Prevents Alveolar Bone Loss in Murine Periodontitis. Front Immunol 9:785
El Kholy, Karim; Freire, Marcelo; Chen, Tsute et al. (2018) Resolvin E1 Promotes Bone Preservation Under Inflammatory Conditions. Front Immunol 9:1300
Van Dyke, T E; Diaz, P I; Moutsopoulos, N et al. (2018) Task Force on Design and Analysis in Oral Health Research: Host-Microbiome Interactions in Dysbiosis. JDR Clin Trans Res 3:6-9
Papathanasiou, E; Trotman, C A; Scott, A R et al. (2017) Current and Emerging Treatments for Postsurgical Cleft Lip Scarring: Effectiveness and Mechanisms. J Dent Res 96:1370-1377
Sima, Corneliu; Montero, Eduardo; Nguyen, Daniel et al. (2017) ERV1 Overexpression in Myeloid Cells Protects against High Fat Diet Induced Obesity and Glucose Intolerance. Sci Rep 7:12848
Freire, Marcelo O; Dalli, Jesmond; Serhan, Charles N et al. (2017) Neutrophil Resolvin E1 Receptor Expression and Function in Type 2 Diabetes. J Immunol 198:718-728
Van Dyke, Thomas E (2017) Pro-resolving mediators in the regulation of periodontal disease. Mol Aspects Med 58:21-36
Agrawal, Madhur; Kern, Philip A; Nikolajczyk, Barbara S (2017) The Immune System in Obesity: Developing Paradigms Amidst Inconvenient Truths. Curr Diab Rep 17:87