Abstract

The focus of this program project is the identification and testing of vaccines for the prevention and treatment of Trypanosoma cruzi infection and Chagas' disease. The protozoan parasite T. cruzi is estimated to infect 16-18 million people and an additional 90 million more at risk of infection. The ultimate consequence of this infection in many individuals, Chagas' disease, is thought to be the single most common cause of congestive heart failure and sudden death in the world and the leading cause of death among young adults in endemic areas of Latin America. Although vector control efforts are making a major impact on the number of new infections in """"""""southern cone"""""""" countries, such efforts do little for the 20 million people already infected. In addition, there is considerable concern about whether vector control alone is a long-term solution to the prevention of T. cruzi infection and Chagas' disease. Vaccines are by far the cheapest and easiest way to reduce morbidity and mortality from most infectious diseases and make considerable sense in an infection such as T. cruzi where the infection is rarely detected in the acute stages and therefore is unlikely to be treated before clinical damage occurs. In this proposal, we describe a genome-based approach using both rational and unbiased techniques for vaccine discovery in T. CRUZI. This approach capitalizes on our understanding of immunity and disease inT. cruzi infection, making use of the strength of the mouse model of T. cruzi infection, the information emerging from genome projects with trypanosomitids, and new technical developments for genome analysis and vaccine delivery. Two specific new approaches will be used in this project for the identification of vaccine candidates in T. cruzi: expression library immunization (ELI) and scanning of DNA microarrays. From this combination of approaches, we expect to identify a minimum of 50 strong vaccine candidates for T. cruzi which will then be testing singly and in combination under various conditions in murine models for protection of mice from both lethal infection and from development of severe disease. We will then firm that such molecules are recognized by humans infected with T. cruzi. The ultimate goal of this project is the identification of a vaccine cocktail that can then be tested in additional models and ultimately, in humans.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
1P01AI044979-01
Application #
2832436
Study Section
Special Emphasis Panel (ZAI1-VSG-M (J1))
Program Officer
Hall, B Fenton
Project Start
1999-09-01
Project End
2004-08-31
Budget Start
1999-09-01
Budget End
2000-08-31
Support Year
1
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Georgia
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
City
Athens
State
GA
Country
United States
Zip Code
30602

  Publications

Castro Eiro, Melisa D; Alvarez, María G; Cooley, Gretchen et al. (2017) The Significance of Discordant Serology in Chagas Disease: Enhanced T-Cell Immunity to Trypanosoma cruzi in Serodiscordant Subjects. Front Immunol 8:1141
Weatherly, D Brent; Peng, Duo; Tarleton, Rick L (2016) Recombination-driven generation of the largest pathogen repository of antigen variants in the protozoan Trypanosoma cruzi. BMC Genomics 17:729
Alvarez, María G; Bertocchi, Graciela L; Cooley, Gretchen et al. (2016) Treatment Success in Trypanosoma cruzi Infection Is Predicted by Early Changes in Serially Monitored Parasite-Specific T and B Cell Responses. PLoS Negl Trop Dis 10:e0004657
Albareda, M Cecilia; Perez-Mazliah, Damián; Natale, M Ailén et al. (2015) Perturbed T cell IL-7 receptor signaling in chronic Chagas disease. J Immunol 194:3883-9
Bustamante, Juan M; Tarleton, Rick L (2014) Potential new clinical therapies for Chagas disease. Expert Rev Clin Pharmacol 7:317-25
Hartley, Ashley N; Cooley, Gretchen; Gwyn, Sarah et al. (2014) Frequency of IFN?-producing T cells correlates with seroreactivity and activated T cells during canine Trypanosoma cruzi infection. Vet Res 45:6
Bustamante, Juan M; Craft, Julie M; Crowe, Byron D et al. (2014) New, combined, and reduced dosing treatment protocols cure Trypanosoma cruzi infection in mice. J Infect Dis 209:150-62
Perez-Mazliah, D E; Alvarez, M G; Cooley, G et al. (2013) Sequential combined treatment with allopurinol and benznidazole in the chronic phase of Trypanosoma cruzi infection: a pilot study. J Antimicrob Chemother 68:424-37
Argüello, Rafael J; Albareda, María C; Alvarez, María G et al. (2012) Inhibitory receptors are expressed by Trypanosoma cruzi-specific effector T cells and in hearts of subjects with chronic Chagas disease. PLoS One 7:e35966
Minning, Todd A; Weatherly, D Brent; Flibotte, Stephane et al. (2011) Widespread, focal copy number variations (CNV) and whole chromosome aneuploidies in Trypanosoma cruzi strains revealed by array comparative genomic hybridization. BMC Genomics 12:139

Showing the most recent 10 out of 32 publications