Abstract

The proposed research is intended to extend our analyses of humoral immune responsiveness at the level of individual B cells isolated in fragment culture. Using fragment cultures derived from carrier-primed irradiated recipients of limiting dilutions of B cells from various sources, it has been possible to demonstrate that in this system: a) a majority of specific donor B cells do respond to give clones antibody forming cells, b) the parameters of both tolerance induction and stimulation including isotype control can be assessed in vitro and at the most sensitive level (responsiveness per B cell), c) the monoclonal antibodies produced are homogeneous and can be scrutinized as to isotype and clonotype (including isofocusing, idiotype, and possibly amino acid sequence), and d) B cells representing various sub-populations including fetal and neonatal B cells can be assessed for competence and diversity. Thus the methods are now available to characterize the adult B cell repertoire and its development and to attempt an evaluation of the genetic and environmental forces which determine its expression. In order to continue this analysis of the B cell repertoire, its acquisition and interactions, we propose these future investigations: A) We will extend our """"""""library"""""""" of identifiable murine clonotypes which currently includes several anti-PC specific clonotypes and neonatal DNP and TNP specific clonotypes to allow a more definitive characterization of these as well as a large variety of clonotypes specific for other determinants. B) We will attempt to increase the yield of monoclonal antibodies by transforming antibody forming cells and attempt to internally label monoclonal antibodies to facilitate defined analyses. C) Finally, we will extend our analyses of the mechanism of B cell triggering, isotype expression (M yields T switch), and tolerance induction with particular emphasis on the role of a) receptor affinity for antigen, b) antigen form, c) specific syngeneic and allogeneic T cells, and d) idiotype specific suppression.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI015797-08
Application #
3126431
Study Section
Immunobiology Study Section (IMB)
Project Start
1978-07-01
Project End
1986-06-30
Budget Start
1985-07-01
Budget End
1986-06-30
Support Year
8
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

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

  Publications

Diaz, Marilyn; Watson, Nicholas B; Turkington, Gene et al. (2003) Decreased frequency and highly aberrant spectrum of ultraviolet-induced mutations in the hprt gene of mouse fibroblasts expressing antisense RNA to DNA polymerase zeta. Mol Cancer Res 1:836-47
Diaz, M; Verkoczy, L K; Flajnik, M F et al. (2001) Decreased frequency of somatic hypermutation and impaired affinity maturation but intact germinal center formation in mice expressing antisense RNA to DNA polymerase zeta. J Immunol 167:327-35
Kline, G H; Hartwell, L; Beck-Engeser, G B et al. (1998) Pre-B cell receptor-mediated selection of pre-B cells synthesizing functional mu heavy chains. J Immunol 161:1608-18
Decker, D J; Linton, P J; Zaharevitz, S et al. (1995) Defining subsets of naive and memory B cells based on the ability of their progeny to somatically mutate in vitro. Immunity 2:195-203
Decker, D J; Kline, G H; Hayden, T A et al. (1995) Heavy chain V gene-specific elimination of B cells during the pre-B cell to B cell transition. J Immunol 154:4924-35
Stillman, C A; Linton, P J; Koutz, P J et al. (1994) Specific immunoglobulin cDNA clones produced from hybridoma cell lines and murine spleen fragment cultures by 3SR amplification. PCR Methods Appl 3:320-31
Linton, P J; Lo, D; Lai, L et al. (1992) Among naive precursor cell subpopulations only progenitors of memory B cells originate germinal centers. Eur J Immunol 22:1293-7
Linton, P J; Klinman, N R (1992) The generation of memory B cells. Semin Immunol 4:3-9
Decker, D J; Boyle, N E; Koziol, J A et al. (1991) The expression of the Ig H chain repertoire in developing bone marrow B lineage cells. J Immunol 146:350-61
Linton, P J; Rudie, A; Klinman, N R (1991) Tolerance susceptibility of newly generating memory B cells. J Immunol 146:4099-104

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