Characterization of the immunodeficiency of RIIIS/J mice: immune response to polysaccharide antigens

Author:

Hiernaux J R1,Baker P J1,McEvoy S J1,Stashak P W1,Fauntleroy M B1,Goidl E A1

Affiliation:

1. Laboratory of Immunogenetics, National Institute of Allergy and Infectious Diseases, Twinbrook II Research Facility, Rockville, Maryland 20852.

Abstract

RIIIS/J mice lack an autosomal dominant gene(s) that influences the magnitude of the antibody response to several polysaccharide antigens of bacterial origin. Low responsiveness is demonstrable whether polysaccharide is administered as a T-helper-cell-independent or -dependent antigen conjugated to an immunogenic carrier; however, RIIIS/J mice make good anti-hapten antibody responses to haptenated polysaccharides. The low antibody responses of RIIIS/J mice to type III pneumococcal polysaccharide do not appear to be the results of an imbalance in the activity of regulatory T lymphocytes. Compared with other strains of mice, RIIIS/J mice elicit low antibody responses to lipopolysaccharide (LPS). They do not develop a cyclic primary or secondary antibody response to Escherichia coli O113 LPS; the latter is not due to a lack of mitogenic response to E. coli O113 LPS. They also produce auto-anti-idiotypic antibody after being immunized with trinitrophenyl-Ficoll.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Immunology,Microbiology,Parasitology

Reference61 articles.

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3. Baker P. J. D. F. Amsbaugh B. Prescott P. W. Stashak and J. A. Rudbach. 1978. Multigenic control of the antibody response to type III pneumococcal polysaccharide and other helper T cell independent antigens p. 67-83. In H. Friedman T. J. Linna and J. E. Prier (ed.) Infection immunity and genetics. University Park Press Baltimore.

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