Abstract

There are two major components of effective vaccines: adjuvants and antigens. The adjuvant for a vaccine must induce the immune responses that are protective, while the antigens must be those against which an immune response can provide protection from infection or disease. Most currently available adjuvants for humans, of which there are very few, induce antibody responses and primarily Th2 T cell responses. For many infections, including M. tuberculosis, Th1 CD4 T cell response and a cytotoxic or cytokine-producing CD8 T cell response are needed. Adjuvants that can induce such responses against subunit proteins and are also safe are urgently needed to tackle the most stubborn infectious diseases. Here, we propose to optimize a promising new adjuvant developed by Statens Serum Institute (SSI), CAF09, which builds on the CAF platform of cationic nanoparticles composed of bioactive lipids. This adjuvant induces both CD4 (Th1, Th17) and CD8 T cells. Optimization of CAF09 formulation and route of vaccination will be performed, using an established subunit vaccine, H56, which was developed by SSI and has been demonstrated to provide protection in several animal models, including non-human primates. Following optimization, the best candidates, based on mouse studies, will be tested for immunogenicity in non-human primates, to provide better translation to humans. The best formulation of CAF09/H56 will be scaled up and toxicity and stability studies will be performed. Finally, one formulation of CAF09/H56, as determined by the iterative studies in mice and monkeys, will be tested in a rigorous non-human primate M. tuberculosis challenge model. These studies will provide the crucial pre-clinical data for moving CAF09/H56 forward into human clinical trials as an improved TB vaccine candidate.

Public Health Relevance

Development of adjuvants that are safe and can induce both CD4 and CD8 T cells is very challenging. However, there are many infectious diseases for which vaccine-induced quality immune responses that include both CD4 and CD8 T cells would improve protection. Tuberculosis, which kills almost 2 million people per year, is exacerbated in the absence of either CD4 or CD8 T cells in non-human primate models. The current vaccines going forward in clinical trials primarily induce only CD4 T cells. Here, we propose to build on exciting data with a unique adjuvant CAF09 to develop this adjuvant for use with a subunit fusion protein (H56) that has previously been demonstrated to provide protection in several animal models. CAF09 induces both CD4 and CD8 T cell responses in mice. We propose to optimize formulation of CAF09, scale-up production, and do toxicity testing. Immunogenicity of H56 formulated with CAF09 will be tested in cynomolgus macaques. Finally, efficacy of H56/CAF09 will be determined in a well-established, rigorous cynomolgus macaque model of tuberculosis. This is a collaboration between Peter Andersen and the Statens Serum Institute, which has a history of adjuvant and vaccine development, and the JoAnne Flynn at University of Pittsburgh School of Medicine who has extensive experience in non-human primate models of tuberculosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI105422-05
Application #
9208083
Study Section
Special Emphasis Panel (ZAI1-SM-M (J1))
Program Officer
Eichelberg, Katrin
Project Start
2013-02-01
Project End
2018-01-31
Budget Start
2017-02-01
Budget End
2018-01-31
Support Year
5
Fiscal Year
2017
Total Cost
$1,133,663
Indirect Cost
$387,778

  Institution

Name
University of Pittsburgh
Department
Genetics
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Cadena, Anthony M; Fortune, Sarah M; Flynn, JoAnne L (2017) Heterogeneity in tuberculosis. Nat Rev Immunol 17:691-702
Woodworth, Joshua S; Andersen, Peter (2016) Reprogramming the T Cell Response to Tuberculosis. Trends Immunol 37:81-83
Billeskov, Rolf; Tan, Esterlina V; Cang, Marjorie et al. (2016) Testing the H56 Vaccine Delivered in 4 Different Adjuvants as a BCG-Booster in a Non-Human Primate Model of Tuberculosis. PLoS One 11:e0161217
Agger, Else Marie (2016) Novel adjuvant formulations for delivery of anti-tuberculosis vaccine candidates. Adv Drug Deliv Rev 102:73-82
Schmidt, Signe Tandrup; Khadke, Swapnil; Korsholm, Karen Smith et al. (2016) The administration route is decisive for the ability of the vaccine adjuvant CAF09 to induce antigen-specific CD8(+) T-cell responses: The immunological consequences of the biodistribution profile. J Control Release 239:107-17
Flynn, JoAnne L; Gideon, Hannah P; Mattila, Joshua T et al. (2015) Immunology studies in non-human primate models of tuberculosis. Immunol Rev 264:60-73
Lin, Philana Ling; Flynn, JoAnne L (2015) CD8 T cells and Mycobacterium tuberculosis infection. Semin Immunopathol 37:239-49
Scanga, Charles A; Flynn, JoAnne L (2014) Modeling tuberculosis in nonhuman primates. Cold Spring Harb Perspect Med 4:a018564
Lindenstrøm, Thomas; Aagaard, Claus; Christensen, Dennis et al. (2014) High-frequency vaccine-induced CD8? T cells specific for an epitope naturally processed during infection with Mycobacterium tuberculosis do not confer protection. Eur J Immunol 44:1699-709