Abstract

Antibodies play an essential role in defending vertebrates against infectious agents and toxins, but, can also induce or exacerbate disease. To better control antibody production, more needs to be learned about the natural mechanisms that regulate B lymphocyte activation and differentiation. In vitro experiments have delineated stimuli that can lead to B cell activation and/or differentiation. These include 1) the crosslinking of B cell surface (s) Ig by antigen or anti-Ig antibody; 2) stimulatory T cell-derived lymphokines; and 3) direct, antigen-mediated interactions between antigen-specific B and T lymphocytes. Little is known, however, about the relative importance of these stimuli in the generation of in vivo antibody responses. To investigate this matter, a system was developed in which the injection of mice with a goat antibody to IgD activates B cells by crosslinking their sIgD, enhances helper cell expression of a receptor for IgD, induces helper T cells to secrete stimulatory lymphokines, and makes possible direct interactions between goat IgG-specific helper cells and sIgD+ B cells. These events stimulate a large, rapid, T cell-dependent polyclonal IgG response. To study the importance of these events in the generation of a polyclonal IgG response this system has been modified by the use of: 1) monoclonal anti-IgD antibodies that differ in their abilities to crosslink IgD and their abilities to be seen as foreign by T cells in different mouse strains; 2) cell transfers between mice that differ only in their Ig allotypes; and 3) alternate mechanisms for the activation of helper T lymphocytes. Issues to be studied include 1) whether the crosslinking of B cell sIgD contributes to the generation of an Ig response in these mice; 2) if so, whether the crosslinking of B cell sIgD contribute to the generation of an IgG response through a) its direct B cell activating effects b) the induction of enhanced T cell IgD receptor expression, and/or c) enhancement of T cell activation; 3) the extent to which crosslinking of B cell sIgD in the absence of sIgD-mediated interactions between adjacent B cells activates these cells; 4) whether a direct anti-IgD antibody-mediated cellular interaction between B cells and activated helper T cells is required for the induction of a polyclonal antibody response in anti-IgD antibody-injected mice; and 5) whether anti-IgD antibody-induced lymphokines can, in the absence of other stimuli, stimulate B cell DNA synthesis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI021328-08
Application #
3131320
Study Section
Immunobiology Study Section (IMB)
Project Start
1984-09-30
Project End
1994-08-31
Budget Start
1992-09-01
Budget End
1994-08-31
Support Year
8
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Henry M. Jackson Fdn for the Adv Mil/Med
Department
Type
DUNS #
City
Rockville
State
MD
Country
United States
Zip Code
20817

  Publications

Greenwald, R J; Urban, J F; Ekkens, M J et al. (1999) B7-2 is required for the progression but not the initiation of the type 2 immune response to a gastrointestinal nematode parasite. J Immunol 162:4133-9
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Gause, W C; Lu, P; Zhou, X D et al. (1996) H. polygyrus: B7-independence of the secondary type 2 response. Exp Parasitol 84:264-73
Urban Jr, J F; Maliszewski, C R; Madden, K B et al. (1995) IL-4 treatment can cure established gastrointestinal nematode infections in immunocompetent and immunodeficient mice. J Immunol 154:4675-84
Finkelman, F D; Holmes, J M; Dukhanina, O I et al. (1995) Cross-linking of membrane immunoglobulin D, in the absence of T cell help, kills mature B cells in vivo. J Exp Med 181:515-25
Lu, P; Zhou, X D; Chen, S J et al. (1995) Requirement of CTLA-4 counter receptors for IL-4 but not IL-10 elevations during a primary systemic in vivo immune response. J Immunol 154:1078-87
Morris, S C; Lees, A; Holmes, J M et al. (1994) Induction of B cell and T cell tolerance in vivo by anti-CD23 mAb. J Immunol 152:3768-76
Squire, C M; Studer, E J; Lees, A et al. (1994) Antigen presentation is enhanced by targeting antigen to the Fc epsilon RII by antigen-anti-Fc epsilon RII conjugates. J Immunol 152:4388-96
Morris, S C; Lees, A; Finkelman, F D (1994) In vivo activation of naive T cells by antigen-presenting B cells. J Immunol 152:3777-85
Lees, A; Finkelman, F; Inman, J K et al. (1994) Enhanced immunogenicity of protein-dextran conjugates: I. Rapid stimulation of enhanced antibody responses to poorly immunogenic molecules. Vaccine 12:1160-6

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