Abstract

Approximately 80% of lymphoblastic lymphomas and 20% of acute lymphoblastic leukemias express phenotypes consistent with prethymic and intrathymic stages of T cell differentiation. Immunophenotyping and, more recently, T cell receptor (TCR) gene rearrangement patterns have been of enormous help in diagnosing and classifying such malignancies. Their exact clonotypic origin, important in diagnosis and therapy, however, has not yet been defined. Utilization of T cell receptor (TCR) variable (V) region-specific nucleotide probes, and corresponding anti- variotypic (V-region-specific) antibodies will be extremely useful in this regard. In addition, anti-variotypic antibodies may be useful as specific therapeutic agents for malignancies of the mature T cell type. The major objective of this proposal is to molecularly characterize the expressed TCR V beta genes of human leukemias/lymphomas and to subsequently attempt to treat such malignancies transplanted into severe combined immunodeficiency disease (scid) mice with anti-V beta-specific antibodies. To accomplish this, a survey on the clonal origin of several human T cell leukemias and lymphomas will first be made by assessing TCR gene rearrangement profiles and, importantly, by identifying their TCR V beta gene usage protection assay. Subsequently, monoclonal antibodies against the most prevalent V beta gene products will be made in mice immunized with a syngeneic lymphoma cell line transfected with corresponding full-length human, or molecularly engineered mouse/human hybrid, V beta genes. Human leukemic cells will be transplanted into scid mice, their growth characteristics established, and the effects of corresponding anti-variotypic antibodies, alone or conjugated with a toxin, will be assessed. These studies will allow the accurate clonal classification of T cell tumors, provide TCR V beta-specific reagents for identification of human TCR V beta usage in malignant and other disorders, and permit the investigation of anti-idiotypic antibodies as specific means of T cell tumor eradication.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA052539-01A1
Application #
3197301
Study Section
Experimental Immunology Study Section (EI)
Project Start
1991-05-15
Project End
1992-04-30
Budget Start
1991-05-15
Budget End
1992-04-30
Support Year
1
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

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

  Publications

Duncan, S R; Elias, D J; Roglic, M et al. (1997) T-cell receptor biases and clonal proliferations in blood and pleural effusions of patients with lung cancer. Hum Immunol 53:39-48
Theofilopoulos, A N; Baccala, R; Gonzalez-Quintial, R et al. (1995) T-cell repertoires in health and disease. Ann N Y Acad Sci 756:53-65
Baccala, R; Vandekerckhove, B A; Jones, D et al. (1993) Bacterial superantigens mediate T cell deletions in the mouse severe combined immunodeficiency-human liver/thymus model. J Exp Med 177:1481-5
Cole, B C; Balderas, R A; Ahmed, E A et al. (1993) Genomic composition and allelic polymorphisms influence V beta usage by the Mycoplasma arthritidis superantigen. J Immunol 150:3291-9
Baccala, R; Smith, L R; Vestberg, M et al. (1992) Mycoplasma arthritidis mitogen. V beta engaged in mice, rats, and humans, and requirement of HLA-DR alpha for presentation. Arthritis Rheum 35:434-42