Abstract

The long term objective of this proposal is to understand the factors that contribute to the virulence and pathogenicity of Bacteroides fragilis, the most important anaerobic pathogen in suppurative intra-abdominal and pelvic infections in human beings. Since this requires a genetic and physiological analysis of the virulence factors, our approach has been to develop new genetic systems for use in B. fragilis in order to identify potential virulence determinants. We are focusing on the aerotolerance of B. fragilis as an important factor in the organisms' ability to survive in oxygenated tissue. We will analyze a set of B. fragilis proteins that are highly expressed only in the presence of oxygen. We will study the control of the synthesis of these oxygen response proteins (ORPs) and attempt to identify global and gene specific regulators. We will also study the process of the shut-off of most B. fragilis proteins normally made during anaerobiosis that occurs when the growing cells are challenged with oxygen. We will continue our studies on the superoxide dismutase of B. fragilis and determine its role in B.fragilis survival in vitro and in vivo. Since we have determined an important role for the B.fragilis neuraminidase in the ability of B.fragilis to grow in two in vivo test systems, we will concentrate on defining the control region of the nanH structural gene and in understanding how its expression is regulated. We will use an adaptation of the TnphoA system that has been used in E.coli to identify exported proteins, in order to study surface proteins of B. fragilis. Since many cell envelope proteins play a role in bacterial pathogenicity, we will use TnCef to identify virulence determinants among B. fragilis surface or exported proteins. Mutants with alterations in potential virulence factors will be tested for their ability to grow in two model systems of B. fragilis infection, the rat granuloma pouch, and CHO or Monika P15 animal cells in culture. We will search for B. fragilis genes that are only expressed when the bacteria are growing in vivo. These genes are likely to play an important role in the establishment and maintenance of B. fragilis infections. To further define the initial steps in B.fragilis infection of the rat pouch, we will perform a histological analysis of the infected pouch at early times after infection. We will determine the location of the infecting B. fragilis cells during the establishment of the anaerobic environment that is required for bacterial growth.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI019499-11
Application #
2060944
Study Section
Special Emphasis Panel (SRC)
Project Start
1990-04-01
Project End
1995-06-30
Budget Start
1994-07-01
Budget End
1995-06-30
Support Year
11
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Mylvaganam, S E; Paterson, Y; Getzoff, E D (1998) Structural basis for the binding of an anti-cytochrome c antibody to its antigen: crystal structures of FabE8-cytochrome c complex to 1.8 A resolution and FabE8 to 2.26 A resolution. J Mol Biol 281:301-22
Mylvaganam, S E; Paterson, Y; Kaiser, K et al. (1991) Biochemical implications from the variable gene sequences of an anti-cytochrome c antibody and crystallographic characterization of its antigen-binding fragment in free and antigen-complexed forms. J Mol Biol 221:455-62
Decker, D J; Boyle, N E; Klinman, N R (1991) Predominance of nonproductive rearrangements of VH81X gene segments evidences a dependence of B cell clonal maturation on the structure of nascent H chains. J Immunol 147:1406-11
Carbone, F R; Bevan, M J (1990) Class I-restricted processing and presentation of exogenous cell-associated antigen in vivo. J Exp Med 171:377-87
Wright, P E; Dyson, H J; Lerner, R A et al. (1990) Antigen-antibody interactions: an NMR approach. Biochem Pharmacol 40:83-8
Heath, W R; Vitiello, A; Sherman, L A (1989) Mapping of epitopes recognized by alloreactive cytotoxic T lymphocytes using inhibition by MHC peptides. J Immunol 143:1441-6
Cooper, H M; Klinman, N R; Paterson, Y (1989) The autoantigenic response to rabbit cytochrome c. Eur J Immunol 19:315-22
Vitiello, A; Heath, W R; Sherman, L A (1989) Consequences of self-presentation of peptide antigen by cytolytic T lymphocytes. J Immunol 143:1512-7
Carbone, F R; Hosken, N A; Moore, M W et al. (1989) Class I MHC-restricted cytotoxic responses to soluble protein antigen. Cold Spring Harb Symp Quant Biol 54 Pt 1:551-5
Hosken, N A; Bevan, M J; Carbone, F R (1989) Class I-restricted presentation occurs without internalization or processing of exogenous antigenic peptides. J Immunol 142:1079-83

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