Abstract

The aim of this research is to develop a safe and effective multivalent vaccine against strains of group A streptococci that trigger acute rheumatic fever and rheumatic heart disease. For this purpose, the chemistry and immunology of the protective as opposed to heart cross-reactive epitopes of streptococcal M protein will be studied in detail. Specific efforts will be directed toward: (1) identifying the protective M protein epitopes predominating among strains of group A streptococci collected from populations in which attacks of rheumatic fever remain high, (2) isolating, purifying and immunochemically analyzing M protein polypeptide fragments for protective and heart cross-reactive epitopes, (3) determining the covalent structure of the aminoterminal and common protective regions of relevant M proteins, (4) synthesizing peptide copies of the amino-terminal regions of selected M proteins, and testing the protective and heart cross-reactive immunogenicity of the peptides conjugated to various carriers in laboratory animals, (5) synthesizing and analyzing tandem hybrids of peptides containing protective epitopes of different M serotypes, and (6) carefully testing the immunogenicity of selected pep M proteins and synthetic peptides as guided by the foregoing studies in human volunteers. The predominant protective epitopes will be determined by M typing, opsonophagocytic and mouse protection tests, and Southern hybridization of the DNA of streptococcal strains with probes prepared from the structural genes encoding M protein under varying conditions of stringency. Purified peptic extracts of rheumatogenic streptococci will be tested for protective and heart cross-reactive immunogenicity in rabbits and mice. The covalent structures of the amino-terminus of the relevant M proteins will be determined by automated sequence analysis. Overlapping peptides will be synthesized, conjugated to various carriers, including pepM24, which has been shown to be devoid of heart cross-reactive epitopes, and tested for type-specific, cross protective and tissue-cross-reactive immunogenicity. Some of the peptides from different M serotypes will be synthesized in tandem in an attempt to produce multivalent hybrid peptides with protective immunogenicity against many serotypes of streptococci. Based on the results obtained in the foregoing studies, the synthetic peptides will be carefully evaluated in humans for protective immunogenicity. These studies should provide fundamental information on the chemistry and immunology of M protein as they relate to protective immunity against rheumatogenic streptococci.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
2R37AI010085-23
Application #
3480541
Study Section
Bacteriology and Mycology Subcommittee 1 (BM)
Project Start
1976-09-01
Project End
1991-08-31
Budget Start
1986-09-01
Budget End
1987-08-31
Support Year
23
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of Tennessee Health Science Center
Department
Type
Schools of Medicine
DUNS #
941884009
City
Memphis
State
TN
Country
United States
Zip Code
38163

  Publications

Courtney, Harry S; Niedermeyer, Shannon E; Penfound, Thomas A et al. (2017) Trivalent M-related protein as a component of next generation group A streptococcal vaccines. Clin Exp Vaccine Res 6:45-49
Dale, James B; Smeesters, Pierre R; Courtney, Harry S et al. (2017) Structure-based design of broadly protective group a streptococcal M protein-based vaccines. Vaccine 35:19-26
Dale, James B; Niedermeyer, Shannon E; Agbaosi, Tina et al. (2015) Protective immunogenicity of group A streptococcal M-related proteins. Clin Vaccine Immunol 22:344-50
Niedermeyer, Shannon E; Penfound, Thomas A; Hohn, Claudia et al. (2014) Group A streptococcus expresses a trio of surface proteins containing protective epitopes. Clin Vaccine Immunol 21:1421-5
Klonoski, Joshua M; Hurtig, Heather R; Juber, Brian A et al. (2014) Vaccination against the M protein of Streptococcus pyogenes prevents death after influenza virus: S. pyogenes super-infection. Vaccine 32:5241-9
Steer, Andrew C; Dale, James B; Carapetis, Jonathan R (2013) Progress toward a global group a streptococcal vaccine. Pediatr Infect Dis J 32:180-2
Dale, James B; Penfound, Thomas A; Chiang, Edna Y et al. (2011) New 30-valent M protein-based vaccine evokes cross-opsonic antibodies against non-vaccine serotypes of group A streptococci. Vaccine 29:8175-8
Penfound, Thomas A; Chiang, Edna Y; Ahmed, Elwaleed A et al. (2010) Protective efficacy of group A streptococcal vaccines containing type-specific and conserved M protein epitopes. Vaccine 28:5017-22
Penfound, Thomas A; Ofek, Itzhak; Courtney, Harry S et al. (2010) The NH(2)-terminal region of Streptococcus pyogenes M5 protein confers protection against degradation by proteases and enhances mucosal colonization of mice. J Infect Dis 201:1580-8
Bronze, Michael S; Dale, James B (2010) Progress in the development of effective vaccines to prevent selected gram-positive bacterial infections. Am J Med Sci 340:218-25

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