Mycobacterium tuberculosis, the primary agent of tuberculosis, infects half of the world's population and is one of the most important diseases in the world from the standpoint of human morbidity and mortality. M. tuberculosis has also emerged as a highly prevalent opportunistic pathogen in AIDS patients. A safe and effective vaccine against M. tuberculosis is sorely needed. The development of such a vaccine is the ultimate goal of the studies proposed in this application. This proposal seeks to identify molecular determinants of cell-mediated immunity and protective immunity to M. tuberculosis in humans. Preliminary investigations have demonstrated the existence of immunoprotective molecules of M. tuberculosis and laid the foundation for further studies aimed at identifying molecules that are candidates for a subunit vaccine. Thus, these studies hold great promise for the development of an effective vaccine against tuberculosis in the near future.
Specific aims of this proposal are to: a) Identify M. tuberculosis proteins which induce cell-mediated immune responses in guinea pigs with pulmonary tuberculosis; b) determine it immunization of guinea pigs with selected M. tuberculosis proteins induces specific cell-mediated and humoral immune responses; c) determine if immunization of guinea pigs with selected M. tuberculosis proteins that induce cell-mediated immune responses establishes protective immunity to aerosol challenge with virulent M. tuberculosis; d) determine optimal conditions for induction of protective immunity by selected M. tuberculosis proteins; e) determine if immunization of guinea pigs with a combination of immunoprotective proteins induces a higher level of protective immunity than single immunogens; f) determine if M. tuberculosis proteins that induce cell-mediated and protective immunity in guinea pigs are expressed in human monocytes infected with M. tuberculosis; g) determine if humans previously exposed to M. tuberculosis develop a cell-mediated immune response to M. tuberculosis proteins that induce cell-mediated and protective immunity in guinea pigs; h) determine if immunoprotective proteins contain immunodominant regions across human MHC types.

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
1R01AI031338-01
Application #
3146305
Study Section
AIDS and Related Research Study Section 5 (ARRE)
Project Start
1991-04-01
Project End
1994-03-31
Budget Start
1991-04-01
Budget End
1992-03-31
Support Year
1
Fiscal Year
1991
Total Cost
Indirect Cost
Name
University of California Los Angeles
Department
Type
Schools of Medicine
DUNS #
119132785
City
Los Angeles
State
CA
Country
United States
Zip Code
90095
Jia, Qingmei; Dillon, Barbara Jane; Masleša-Gali?, Saša et al. (2017) Listeria-vectored vaccine expressing the Mycobacterium tuberculosis 30 kDa major secretory protein via the constitutively active prfA* regulon boosts BCG efficacy against tuberculosis. Infect Immun :
Gillis, Thomas P; Tullius, Michael V; Horwitz, Marcus A (2014) rBCG30-induced immunity and cross-protection against Mycobacterium leprae challenge are enhanced by boosting with the Mycobacterium tuberculosis 30-kilodalton antigen 85B. Infect Immun 82:3900-9
Horwitz, Marcus A; Harth, Günter; Dillon, Barbara Jane et al. (2009) Commonly administered BCG strains including an evolutionarily early strain and evolutionarily late strains of disparate genealogy induce comparable protective immunity against tuberculosis. Vaccine 27:441-5
Hoft, Daniel F; Blazevic, Azra; Abate, Getahun et al. (2008) A new recombinant bacille Calmette-Guerin vaccine safely induces significantly enhanced tuberculosis-specific immunity in human volunteers. J Infect Dis 198:1491-501
Tullius, Michael V; Harth, Gunter; Maslesa-Galic, Sasa et al. (2008) A Replication-Limited Recombinant Mycobacterium bovis BCG vaccine against tuberculosis designed for human immunodeficiency virus-positive persons is safer and more efficacious than BCG. Infect Immun 76:5200-14
Horwitz, Marcus A; Harth, Gunter; Dillon, Barbara Jane et al. (2006) A novel live recombinant mycobacterial vaccine against bovine tuberculosis more potent than BCG. Vaccine 24:1593-600
Horwitz, Marcus A; Harth, Gunter; Dillon, Barbara Jane et al. (2006) Extraordinarily few organisms of a live recombinant BCG vaccine against tuberculosis induce maximal cell-mediated and protective immunity. Vaccine 24:443-51
Horwitz, Marcus A (2005) Recombinant BCG expressing Mycobacterium tuberculosis major extracellular proteins. Microbes Infect 7:947-54
Harth, Gunter; Maslesa-Galic, Sasa; Tullius, Michael V et al. (2005) All four Mycobacterium tuberculosis glnA genes encode glutamine synthetase activities but only GlnA1 is abundantly expressed and essential for bacterial homeostasis. Mol Microbiol 58:1157-72
Horwitz, Marcus A; Harth, Gunter; Dillon, Barbara Jane et al. (2005) Enhancing the protective efficacy of Mycobacterium bovis BCG vaccination against tuberculosis by boosting with the Mycobacterium tuberculosis major secretory protein. Infect Immun 73:4676-83

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