Abstract

The need to develop new vaccines against mucosal pathogens has compelled a search for adjuvants thatcan effectively stimulate mucosal immunity to vaccine proteins, most of which are poor immunogens. Toll-like receptors (TLRs) and gangliosides are considered 'adjuvant receptors' because their interaction withcertain classes of noxious microbial molecules generates potent immunomodulatory signals in antigen-presenting cells (APCs) that mobilize adaptive immunity. An ideal adjuvant should thus stimulate adjuvantreceptors without, however, inducing toxic effects. This proposal will investigate the adjuvant activities of anovel ganglioside-binding TLR2 agonist, recently identified by our group. The molecule under investigationis the pentameric B subunit of a unique E. coli enterotoxin, designated Type Mb(LT-llb) and quite differentfrom Type I enterotoxins such as cholera toxin. In contrast to the intact toxin, the B subunit (designated LT-llb-B) induces TLR2-dependent activation of transcription factor NF-KB, which plays a central role in theinduction of immunoregulatory cytokines and costimulatory molecules on APCs, such as dendritic cells. Theoverall hypothesis is that LT-llb-B exhibits immunomodulatory activity, which requires the cooperation ofGD1a ganglioside and TLR2, promotes antigen-presenting cell function, and induces mucosal immunity. Wethus aim to elucidate the immunomodulatory mechanisms of LT-llb-B and demonstrate its mucosaladjuvanticity. Specifically, using immunological, biophysical, and cell imaging techniques, we will determinecooperative interactions between gangliosides and TLR2 in response to LT-llb-B, and the importance ofthese interactions in upregulating dendritic cell-mediated functional costimulation to CD4+T cells. Moreover,it will be determined if these adjuvant mechanisms of LT-llb-B correlate with induction of mucosal adjuvantactivity in vivo. The proposed studies are supported by a plethora of preliminary findings and are facilitatedby the availability of (a) engineered wild-type and single point substitution mutants of LT-II molecules, (b)model cell systems where expression of receptors of interest is manipulated and (c) a well-establishedmouse mucosal immunization model. Using these models and state-of-the-art interdisciplinary techniques,the generated data will form the basis for our ultimate objective which is to establish LT-llb-B as a safe andeffective adjuvant in vaccine formulations against oral or other mucosal pathogens.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
7R01DE017138-08
Application #
8388433
Study Section
Oral, Dental and Craniofacial Sciences Study Section (ODCS)
Program Officer
Burgoon, Penny W
Project Start
2006-02-01
Project End
2015-08-31
Budget Start
2012-01-01
Budget End
2012-08-31
Support Year
8
Fiscal Year
2011
Total Cost
$388,491
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Microbiology/Immun/Virology
Type
Schools of Dentistry
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Lee, Chang Hoon; Hajishengallis, George; Connell, Terry D (2017) Dendritic Cell-Mediated Mechanisms Triggered by LT-IIa-B5, a Mucosal Adjuvant Derived from a Type II Heat-Labile Enterotoxin of Escherichia coli. J Microbiol Biotechnol 27:709-717
Maekawa, T; Kulwattanaporn, P; Hosur, K et al. (2017) Differential Expression and Roles of Secreted Frizzled-Related Protein 5 and the Wingless Homolog Wnt5a in Periodontitis. J Dent Res 96:571-577
Hajishengallis, George; Moutsopoulos, Niki M; Hajishengallis, Evlambia et al. (2016) Immune and regulatory functions of neutrophils in inflammatory bone loss. Semin Immunol 28:146-58
Hajishengallis, George; Hajishengallis, Evlambia; Kajikawa, Tetsuhiro et al. (2016) Complement inhibition in pre-clinical models of periodontitis and prospects for clinical application. Semin Immunol 28:285-91
Hajishengallis, George; Lambris, John D (2016) More than complementing Tolls: complement-Toll-like receptor synergy and crosstalk in innate immunity and inflammation. Immunol Rev 274:233-244
Duan, X; Gleason, R C; Li, F et al. (2016) Sex dimorphism in periodontitis in animal models. J Periodontal Res 51:196-202
Olsen, Ingar; Hajishengallis, George (2016) Major neutrophil functions subverted by Porphyromonas gingivalis. J Oral Microbiol 8:30936
Hajishengallis, George; Lamont, Richard J (2016) Dancing with the Stars: How Choreographed Bacterial Interactions Dictate Nososymbiocity and Give Rise to Keystone Pathogens, Accessory Pathogens, and Pathobionts. Trends Microbiol 24:477-489
Maekawa, Tomoki; Briones, Ruel A; Resuello, Ranillo R G et al. (2016) Inhibition of pre-existing natural periodontitis in non-human primates by a locally administered peptide inhibitor of complement C3. J Clin Periodontol 43:238-49
Mastellos, D C; Ricklin, D; Hajishengallis, E et al. (2016) Complement therapeutics in inflammatory diseases: promising drug candidates for C3-targeted intervention. Mol Oral Microbiol 31:3-17

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