Abstract

The mechanisms by which an individual generates and regulates a multitude of antibody-producing cells is being studied. The difficulty in this type of study is the enormous heterogeneity that exists within the potential antibody-producing cell repertoire. A small portion of this repertoire is being defined by immortalizing antibody-producing cells (specific for the hapten phthalate) by cell fusion analysis. Our efforts to define the secondary response to this hapten were initially frustrated by the apparent unlimited heterogeneity of this response (perhaps generated in part by random somatic mutations within the genes coding for the variable portions of the light and heavy immunoglobulin chains). Our recent efforts have focused upon the antibody-producing clones that appear very early (3 to 4 days) after a single immunization with a phthalate-protein conjugate. The rationale for this shift in focus was the possibility that fewer clones were stimulated early in the response and that these clones would represent conserved immunoglobulin gene products. Our findings are consistent with this assumption, and our endeavors have led to the generation of a hybridoma clone 2E9 that has had a significant positive impact upon our research program. The 2E9 hybrid clone secretes a phthalate-specific antibody whose idiotype appears repeatedly in cell fusion analysis of hybrid clones secreting anti-phthalate antibodies with either mu or gammal heavy chain isotypes. Analysis of the primary and secondary response sera of BAL8/c mice (as well as several other strains) indicates that the 2E9 clonotype represents a major conserved phthalate-specific antibody-forming cell family. The significance of this finding to our program is that it enables us to monitor the effects of various perturbations upon the expression of this conserved clonotype. Earlier studies with a response of mice to dextran (a response that occurs without a requirement of T cells) demonstrated the significance of idiotype recognition in the regulation of expression of a dextran-specific clonotype. We are now able to determine if regulation of phthalate-specific clonotypes (a response requiring T cells) similarily involves idiotype recognition by regulatory cells. (LB)

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA025253-09
Application #
3166779
Study Section
Allergy and Immunology Study Section (ALY)
Project Start
1979-03-01
Project End
1988-07-31
Budget Start
1987-08-01
Budget End
1988-07-31
Support Year
9
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
Roswell Park Cancer Institute Corp
Department
Type
DUNS #
City
Buffalo
State
NY
Country
United States
Zip Code
14263

  Publications

Cuenca, R E; Takita, H; Bankert, R (1996) Orthotopic engraftment of human lung tumours in SCID mice for the study of metastasis. Surg Oncol 5:85-91
Falkenberg, S; Winter, D; Bankert, R B (1995) Transient dominance of the early primary immune response by a highly conserved B-cell clone that is distinguished by its lack of memory, high threshold of activation, and a high affinity. Cell Immunol 160:123-31
Alosco, T; Croy, B A; Gansbacher, B et al. (1993) Antitumor response independent of functional B or T lymphocytes induced by the local and sustained release of interleukin-2 by the tumor cells. Cancer Immunol Immunother 36:364-72
Lou, S C; Winter, D; Mayers, G L et al. (1992) Nucleotide sequence of messenger RNA encoding VHDJH and VKJK of a highly conserved idiotype-defined primary response anti-hapten antibody. J Immunol 149:3944-52
Williams, S S; Umemoto, T; Kida, H et al. (1992) Engraftment of human peripheral blood leukocytes into severe combined immunodeficient mice results in the long term and dynamic production of human xenoreactive antibodies. J Immunol 149:2830-6
Chen, F A; Repasky, E A; Bankert, R B (1991) Human lung tumor-associated antigen identified as an extracellular matrix adhesion molecule. J Exp Med 173:1111-9
Ghosh, S K; White, L M; Ghosh, R et al. (1990) Vaccination with membrane-associated idiotype provides greater and more prolonged protection of animals from tumor challenge than the soluble form of idiotype. J Immunol 145:365-70
Drake, J R; Repasky, E A; Bankert, R B (1989) Endocytosis of antigen, anti-idiotype, and anti-immunoglobulin antibodies and receptor re-expression by murine B cells. J Immunol 143:1768-76
Chen, F A; Repasky, E A; Takita, H et al. (1989) Cell surface glycoprotein associated with human lung tumors that is similar to but distinct from the epidermal growth factor receptor. Cancer Res 49:3642-9
Bankert, R B; Yokota, S; Ghosh, S K et al. (1989) Immunospecific targeting of cytosine arabinonucleoside-containing liposomes to the idiotype on the surface of a murine B-cell tumor in vitro and in vivo. Cancer Res 49:301-8

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