Abstract

Although the influenza vaccine has been used for over 60 years, the current vaccination strategy against influenza A and B viruses is vulnerable to the unanticipated emergence of epidemic strains that are poorly matched by the vaccine. Epidemics of seasonal influenza and increased circulation of avian influenza virus subtypes constitute a significant healthcare problem in all regions of the world, including the U.S. The annually recommended vaccination is the principal means of controlling influenza epidemics. However, the current licensed vaccines (trivalent inactivated or live, attenuated trivalent virus vaccines) provide protection only against the strains that are matched with the vaccine composition. There is no influenza pandemic vaccine available to the general public. In addition, the current vaccine production is based on egg substrates and would not meet the surge demand in vaccination during a pandemic outbreak. Therefore, development of influenza vaccines with improved protective efficacy against influenza virus is an imperative. Zetra's uniquely engineered adjuvant-containing viral nanoparticles (cVLPs) provided proof-of-concept that a broadly cross-protective, non-replicating vaccine with the possibility of cross reactivity with other influenza subtypes A and B, can be developed by the company's proprietary technology. The protective immune responses induced by these cVLPs have been maintained at high levels in mice for over 14-months. This desirable quality of our vaccines provides a potential to avoid the need to change the seasonal vaccine formulation every year. Importantly, a single immunization induced protective immunity against a high dose of challenge virus. A major goal of this project is to develop and evaluate novel adjuvant-containing influenza cVLPs vaccines against influenza virus in order to enhance broadly cross protective and long-lasting immunity. Granulocyte-macrophage colony-stimulating factor (GM-CSF) is known to increase the immunogenicity of various co-administered antigens and is considered as an adjuvant appropriate for human use. We propose the novel approach to use GM-CSF in a membrane-anchored form in VLPs with influenza antigens. We have already developed chimeric influenza VLPs incorporating GM-CSF which show desirable vaccine qualities. Cross-protection as well as heterosubtypic protection models have been well established in our laboratory for seasonal influenza. In Phase I of this project, we will determine the cross-protective efficacy including heterosubtypic immunity induced by chimeric influenza VLPs containing the immunostimulatory molecule, GM-CSF, in well-established mouse and ferret models. The physical co-localization of the cytokine adjuvant and antigen in the same VLP is important to increase the efficacy of our novel vaccines. Our approach to development of a safe and effective vaccine that induces broadly cross protective immunity against influenza viruses will have a significant impact on public health in general.

Public Health Relevance

Epidemics of seasonal influenza and increased circulation of avian influenza virus subtypes constitute a significant healthcare problem in all regions of the world, including the U.S. The annually recommended vaccination is the principal means of controlling influenza epidemics. However, the current licensed vaccines (trivalent inactivated or live, attenuated trivalent virus vaccines) provide protection only against the strains that are matched with the vaccine composition. The goal of this project is the development of an engineered adjuvant-containing and improved influenza vaccine that will induce broadly cross-protective and long-lasting immunity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Small Business Innovation Research Grants (SBIR) - Phase I (R43)
Project #
5R43AI081385-02
Application #
7924892
Study Section
Special Emphasis Panel (ZRG1-IMM-K (12))
Program Officer
Salomon, Rachelle
Project Start
2009-09-01
Project End
2011-08-31
Budget Start
2010-09-01
Budget End
2011-08-31
Support Year
2
Fiscal Year
2010
Total Cost
$299,999
Indirect Cost

  Institution

Name
Zetra Biologicals, LLC
Department
Type
DUNS #
791285062
City
Tucker
State
GA
Country
United States
Zip Code
30084

  Publications

Quan, Fu-Shi; Kim, Min-Chul; Lee, Byeong-Jae et al. (2012) Influenza M1 VLPs containing neuraminidase induce heterosubtypic cross-protection. Virology 430:127-35
Shastri, Prathap Nagaraja; Kim, Min-Chul; Quan, Fu-Shi et al. (2012) Immunogenicity and protection of oral influenza vaccines formulated into microparticles. J Pharm Sci 101:3623-35
Kang, Sang-Moo; Kim, Min-Chul; Compans, Richard W (2012) Virus-like particles as universal influenza vaccines. Expert Rev Vaccines 11:995-1007
Kim, Yeu-Chun; Song, Jae-Min; Lipatov, Aleksandr S et al. (2012) Increased immunogenicity of avian influenza DNA vaccine delivered to the skin using a microneedle patch. Eur J Pharm Biopharm 81:239-47
Kang, Sang-Moo; Yoo, Dae-Goon; Kim, Min-Chul et al. (2011) MyD88 plays an essential role in inducing B cells capable of differentiating into antibody-secreting cells after vaccination. J Virol 85:11391-400
Quan, Fu-Shi; Li, Zhu-Nan; Kim, Min-Chul et al. (2011) Immunogenicity of low-pH treated whole viral influenza vaccine. Virology 417:196-202
Kang, S M; Song, J M; Compans, R W (2011) Novel vaccines against influenza viruses. Virus Res 162:31-8
Song, Jae-Min; Choi, Chi-Won; Kwon, Sang-Oh et al. (2011) Proteomic characterization of influenza H5N1 virus-like particles and their protective immunogenicity. J Proteome Res 10:3450-9