Abstract

Among the pathogens thought to represent the greatest threat as bioweapons are Bacillus anthracis, Francisella tularensis and smallpox, which are all CDC designated category A pathogens. As bioweapons they are particularly troublesome because they use the pulmonary route and produce diseases that are unusually difficult to diagnose and treat. Further, we know very little about the interaction of these pathogens with the lung environment. The two primary protective options available are: 1) development of vaccines that induce effective acquired immunity against lung infections and/or 2) development of therapeutics that enhance innate immunity. Understanding the mechanisms by which innate and acquired immunity protect against pulmonary challenge with category A pathogens is critical for developing new therapeutics. None of these pulmonary biothreat infections have a high enough incidence in nature to allow us to determine efficacy using standard epidemiological and statistical analysis. Therefore, we must rely heavily on well characterized animal models. We have developed murine pulmonary models for anthrax, virulent tularemia and cowpox virus. We have partnered with Lovelace Respiratory Research Institute to address the interactions of these pathogens with the lung. The Project Leaders of the projects and Cores bring complementary expertise to this Program Project that will provide significant synergy for all of the projects and their aims. Project 1 (Lipscomb) will use defined B. anthracis mutants to investigate the role of the primary virulence factors in dissemination from the lung and induction of end organ damage in murine and nonhuman primate models of inhalation anthrax. It will also investigate the role of alveolar macrophages and complement in preventing dissemination. Project 2 (Pickup) will address the host factors responsible for protection from a pulmonary orthopox virus infection and define the role of poxvirus accessory proteins in pulmonary infections. Project 3 (Lyons) will use a recently developed murine model of LVS vaccination induced protection against a pulmonary infection with Biovar A F. tularensis to define the immune mechanisms responsible for protection. Protective mechanisms identified in the murine model will be compared with those identified in an aerosol exposed nonhuman primate model. In partnership with Macrogenics, we will use Expression Library Immunization to interrogate the F. tularensis genome for vaccine candidates.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
1P01AI056295-01A1
Application #
6851422
Study Section
Special Emphasis Panel (ZAI1-AR-I (S1))
Program Officer
Nabavi, Nasrin N
Project Start
2005-07-01
Project End
2010-06-30
Budget Start
2005-07-01
Budget End
2006-06-30
Support Year
1
Fiscal Year
2005
Total Cost
$1,890,737
Indirect Cost

  Institution

Name
University of New Mexico
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
868853094
City
Albuquerque
State
NM
Country
United States
Zip Code
87131

  Publications

Hutt, Julie A; Lovchik, Julie A; Drysdale, Melissa et al. (2014) Lethal factor, but not edema factor, is required to cause fatal anthrax in cynomolgus macaques after pulmonary spore challenge. Am J Pathol 184:3205-16
Lovchik, Julie A; Drysdale, Melissa; Koehler, Theresa M et al. (2012) Expression of either lethal toxin or edema toxin by Bacillus anthracis is sufficient for virulence in a rabbit model of inhalational anthrax. Infect Immun 80:2414-25
Mara-Koosham, Gopi; Hutt, Julie A; Lyons, C Rick et al. (2011) Antibodies contribute to effective vaccination against respiratory infection by type A Francisella tularensis strains. Infect Immun 79:1770-8
Hansen, Spencer J; Rushton, John; Dekonenko, Alexander et al. (2011) Cowpox virus inhibits human dendritic cell immune function by nonlethal, nonproductive infection. Virology 412:411-25
Chand, Hitendra S; Schuyler, Mark; Joste, Nancy et al. (2010) Anti-IgE therapy results in decreased myeloid dendritic cells in asthmatic airways. J Allergy Clin Immunol 125:1157-1158.e5
Lipscomb, Mary F; Hutt, Julie; Lovchik, Julie et al. (2010) The pathogenesis of acute pulmonary viral and bacterial infections: investigations in animal models. Annu Rev Pathol 5:223-52
Borovkov, Alex Y; Loskutov, Andrey V; Robida, Mark D et al. (2010) High-quality gene assembly directly from unpurified mixtures of microarray-synthesized oligonucleotides. Nucleic Acids Res 38:e180
Wu, Terry H; Zsemlye, Jason L; Statom, Gloria L et al. (2009) Vaccination of Fischer 344 rats against pulmonary infections by Francisella tularensis type A strains. Vaccine 27:4684-93
Collazo, Carmen M; Meierovics, Anda I; De Pascalis, Roberto et al. (2009) T cells from lungs and livers of Francisella tularensis-immune mice control the growth of intracellular bacteria. Infect Immun 77:2010-21
Hahn, Andrew C; Lyons, C Rick; Lipscomb, Mary F (2008) Effect of Bacillus anthracis virulence factors on human dendritic cell activation. Hum Immunol 69:552-61

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