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Laboratory of Molecular Microbial Immunity
By using this unique mouse model and periodontal immunity-based expression cloning strategy, we have recently discovered: i) critical human T-cell-associated osteoclastogenic factor, Receptor Activator of NF-kB Ligand (RANKL), that controls osteoclast differentiation, activation and interactions with RANK and/or OPG (osteoprotegerin) molecules to regulate alveolar bone loss and remodeling in vivo, and ii) novel microbial virulence factors (CagE & OMP1 of Actinobacillus actinomycetemcomitans-Aa, a key human periodontal pathogen forming the “infectious biofilm”) associated with tissue inflammation and destructive immunity in active periodontitis in vivo. Current research projects include:
2. Anaerobes: antigen-presenting cells (APC): T cell interactions during early phase of infection and biofilm formation 3. Exacerbated or aberrant host immunity to microbial infections associated with type-1 diabetes by using the NOD mouse model and the subsequent molecular interactions of T-cell-mediated immuno-regulation associated with bone remodeling
6. QC-PCR in clinical diagnostic applications 7. Clinical application(s) of RANKL/RANK and OPG in human periodontitis Recent Publications and Presentations
NIDCR-NIH; CIHR-Canadian Institute of Health Research, Canada; Ministry of Health of Ontario, Ontario, Canada; London Health Sciences Center, London, Canada.
Andy Y-T. Teng, DDS, MS, Ph.D |
Human
periodontal disease (e.g., periodontitis) results from interactions
between specific sub-gingival biofilm and host immune/inflammatory
response; and it is a prime cause and global epidemic of tooth loss
in adults. Patients who have periodontits may demonstrate increased
risk for developing coronary heart diseases, diabetes, bacterial
pneumonia and pre-term low birth-weigh babies. 
1.
Human immune-microbial interactions in vivo: humanized
NOD/SCID mouse model engrafted by immunocompetent human peripheral
blood leukocytes to study G(-) anaerobic infections on mucosal surfaces
such as human periodontitis or infections in oral cavity
4. The cellular and molecular interactions between specific
bacterial virulence factors (i.e., CagE homologue and OMP1
of Actinobacillus actinomycetemcomitans) and the host immunity using
humanized mouse model or genetically altered mouse models
Funding sources:
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