Abstract

Role of helper T cells in B cell Response: Comparison of naive and memory B cells. Long-lived protective immunity to pathogens depends on the generation, during the first exposure, of memory lymphocytes which are specialized to respond quickly and effectively to re-encounter with the same pathogen. Naive B cells specific for any particular pathogen are present at low frequencies and their activation and proliferation are essential for effective primary Antibody (Ab) response. After immunization, memory B cells are present at increased frequencies, they have often switched from production of IgM Ab to production of more effective isotypes such as IgG and the Ab they now make is of much higher affinity for the antigens seen during the primary response. Other features of naive and memory B cells are much less clear. A major goal in this proposal is to devise methods to identify and isolate naive and memory B cells, using mice transgenic for the B cell Ab Receptor. We will then determine the properties of naive and memory B, including their lifespans, in vivo turnover and capacity to home to key lymphoid tissues. We will investigate in detail the requirements of naive and memory B cells for T cell help, including the role of the direct recognition of the B cell by the T cell, the role of interactions between so-called """"""""costimulatory"""""""" molecules on the two cells and the role of cytokines produced by helper T cells. Different T cell subsets will be compared for their ability to help, including newly defined subsets of CD8 T cells making distinct patterns of cytokines. We will also examine whether the role of the helpers and their products includes rescuing the B cells from programmed cell death. In later stages of the grant, we will use the information obtained above to examine the role of cytokines and T cell subsets in the in vivo primary response and in generation of B cell memory and we will develop in vitro models to study the generation of B cell memory and the factors which regulate that process. These studies should provide important new insights into the most effective procedures for generating primary responses to new antigens, for generating protective immunity and for eliciting an optimum response after priming.

  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 #
2R37AI022125-11
Application #
2061712
Study Section
Experimental Immunology Study Section (EI)
Project Start
1985-09-30
Project End
1996-07-31
Budget Start
1995-08-01
Budget End
1996-07-31
Support Year
11
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of California San Diego
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
077758407
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Kamperschroer, Cris; Roberts, Deborah M; Zhang, Yongqing et al. (2008) SAP enables T cells to help B cells by a mechanism distinct from Th cell programming or CD40 ligand regulation. J Immunol 181:3994-4003
Kamperschroer, Cris; Dibble, John P; Meents, Dana L et al. (2006) SAP is required for Th cell function and for immunity to influenza. J Immunol 177:5317-27
Harris, D P; Haynes, L; Sayles, P C et al. (2000) Reciprocal regulation of polarized cytokine production by effector B and T cells. Nat Immunol 1:475-82
Rogers, P R; Dubey, C; Swain, S L (2000) Qualitative changes accompany memory T cell generation: faster, more effective responses at lower doses of antigen. J Immunol 164:2338-46
Swain, S L (2000) CD4 T-cell memory can persist in the absence of class II. Philos Trans R Soc Lond B Biol Sci 355:407-11
Carter, L L; Zhang, X; Dubey, C et al. (1998) Regulation of T cell subsets from naive to memory. J Immunother 21:181-7
Carter, L L; Swain, S L (1998) From naive to memory. Development and regulation of CD4+ T cell responses. Immunol Res 18:1-13
Dubey, C; Croft, M; Swain, S L (1996) Naive and effector CD4 T cells differ in their requirements for T cell receptor versus costimulatory signals. J Immunol 157:3280-9
Croft, M; Swain, S L (1995) Recently activated naive CD4 T cells can help resting B cells, and can produce sufficient autocrine IL-4 to drive differentiation to secretion of T helper 2-type cytokines. J Immunol 154:4269-82
Dubey, C; Croft, M; Swain, S L (1995) Costimulatory requirements of naive CD4+ T cells. ICAM-1 or B7-1 can costimulate naive CD4 T cell activation but both are required for optimum response. J Immunol 155:45-57

Showing the most recent 10 out of 31 publications