Abstract

The eradication of global pathogens responsible for endemic and pandemic diseases hinges upon the development of effective vaccines. This is certainly the case for malaria. However, our inability to elicit ?strong and long-lasting? protective T cell responses, particularly CD8+ T cell responses, has been a major obstacle to successful vaccine development. Accordingly, adjuvant technologies will likely be critical not only to overcome pre-existing immunity to viral vaccine vectors but also to further enhance vaccine immunogenicity. Our previous studies have demonstrated that a CD1d molecule-binding, natural killer T (NKT) cell ligand, a-galactosylceramide (a-GalCer), can enhance protective CD8+ T cell responses elicited by murine malaria vaccines, including a recombinant adenovirus expressing a malarial antigen. In collaboration with two eminent chemistry groups directed by Dr. Chi-Huey Wong and Dr. Richard Franck, we have successfully identified several a- GalCer analogs that act as NKT cell ligands. In this proposal, we aim to first screen a focused library of one hundred a-GalCer analogs that we have recently generated, and then select a smaller panel of candidate glycolipids based on the in vitro cytokine production profiles they elicit upon cultivation with murine or human NKT cells. We will also determine the in vivo cytokine production profiles elicited by the selected glycolipids upon administration to mice. These in vitro and in vivo screening processes will lead us to choose a dozen of promising candidate glycolipids that display strong Th1-biased, Th2-biased, or bipolar activities.
Our second aim will be to determine the magnitude of adjuvant effect that each of these newly identified glycolipids contributes to the immunogenicity of a malaria vaccine. We will subsequently characterize the anti-malarial CD8+ T cell responses augmented by the glycolipids in a mouse model. Our third and final aim will be to determine the organs and cell types that present the malarial antigen to CD8+ T cells, and subsequently to uncover the mechanisms underlying the adjuvant effects of a-GalCer and its analogs. This work will involve the utilization of a recombinant adenovirus, co-expressing a malarial antigen and green fluorescent protein (GFP). Project Narrative Malaria continues to pose a grave threat to the global community and in particular to adults and children traveling to or living in tropical and subtropical regions of the world. The purpose of this proposal is to develop a novel strategy to enhance the efficacy of malaria vaccines by employing glycolipids as immuno-enhancing compounds or ?adjuvants.? The development of a suitable malaria vaccine/glycolipid adjuvant combination would have the potential to decrease the incidence of malaria and diminish the morbidity and mortality attributable to this pathogen.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
High Priority, Short Term Project Award (R56)
Project #
1R56AI070258-01A2
Application #
7568386
Study Section
Vaccines Against Microbial Diseases (VMD)
Program Officer
Ferguson, Stacy E
Project Start
2008-04-01
Project End
2010-03-31
Budget Start
2008-04-01
Budget End
2010-03-31
Support Year
1
Fiscal Year
2008
Total Cost
$478,188
Indirect Cost

  Institution

Name
Aaron Diamond AIDS Research Center
Department
Type
DUNS #
786658872
City
New York
State
NY
Country
United States
Zip Code
10016

  Publications

Fernandez-Arias, Cristina; Arias, Clemente F; Zhang, Min et al. (2018) Modeling the effect of boost timing in murine irradiated sporozoite prime-boost vaccines. PLoS One 13:e0190940
Li, Xiangming; Huang, Jing; Kawamura, Akira et al. (2017) Co-localization of a CD1d-binding glycolipid with an adenovirus-based malaria vaccine for a potent adjuvant effect. Vaccine 35:3171-3177
Zhang, Min; Gallego-Delgado, Julio; Fernandez-Arias, Cristina et al. (2017) Inhibiting the Plasmodium eIF2? Kinase PK4 Prevents Artemisinin-Induced Latency. Cell Host Microbe 22:766-776.e4
Coelho-Dos-Reis, Jordana G; Huang, Jing; Tsao, Tiffany et al. (2016) Co-administration of ?-GalCer analog and TLR4 agonist induces robust CD8(+) T-cell responses to PyCS protein and WT-1 antigen and activates memory-like effector NKT cells. Clin Immunol 168:6-15
Li, Xiangming; Kawamura, Akira; Andrews, Chasity D et al. (2015) Colocalization of a CD1d-Binding Glycolipid with a Radiation-Attenuated Sporozoite Vaccine in Lymph Node-Resident Dendritic Cells for a Robust Adjuvant Effect. J Immunol 195:2710-21
Shimizu, Kanako; Sato, Yusuke; Shinga, Jun et al. (2014) KLRG+ invariant natural killer T cells are long-lived effectors. Proc Natl Acad Sci U S A 111:12474-9
Avci, Fikri Y; Li, Xiangming; Tsuji, Moriya et al. (2013) Carbohydrates and T cells: a sweet twosome. Semin Immunol 25:146-51
Padte, Neal N; Boente-Carrera, Mar; Andrews, Chasity D et al. (2013) A glycolipid adjuvant, 7DW8-5, enhances CD8+ T cell responses induced by an adenovirus-vectored malaria vaccine in non-human primates. PLoS One 8:e78407
Li, Xiangming; Polacino, Patricia; Garcia-Navarro, Raquel et al. (2012) Peripheral blood invariant natural killer T cells of pig-tailed macaques. PLoS One 7:e48166
Webb, Tonya J; Li, Xiangming; Giuntoli 2nd, Robert L et al. (2012) Molecular identification of GD3 as a suppressor of the innate immune response in ovarian cancer. Cancer Res 72:3744-52

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