Abstract

We wish to test the hypothesis that the development of B cell lymphomas in humans represents a multistep process which begins in the bone marrow. This idea stemmed from studies of B and T cell malignancies in chickens and mice, and we have obtained support for it in previous studies of humans with pre-B, B and plasma cell malignancies. It contrasts with the prevailing view that B cell lymphomas arise in the lymph node; the nodular lymphomas having as their origin a subpopulation of target cells in germinal centers. In the present studies we will examine the extent of clonal involvement in patients with nodular B cell lymphomas. Cell hybridization techniques will be used to produce two types of monoclonal anti-idiotype (Id) antibodies: One specific for idiotypic determinants expressed by complete immunoglobulin molecules and others specific for V(H) idiotopes expressed on the isolated Mu heavy chains made by the B lymphoma. The former will be used to trace the distribution of the B cells belonging to the neoplastic clone in lymph node, blood and bone marrow tissue samples. The anti-V(H) Id will be used to search for members of the neoplastic clones among the pre-B cell population in the bone marrow. After determining the extent of clonal involvement, neoplastic cells and normal B cells will be isolated from each of the involved tissues and pre-B cells isolated from bone marrow. These subpopulations of cells will then be separately examined by cytogenetic techniques for chromosomal abnormalities, and restriction fragments of the cellular DNA will be analyzed with heavy and light chain gene cDNA probes to determine immunoglobulin gene rearrangements and clonality. Other studies will address the expression of cellular oncogenes in the different subpopulations. In this way we hope to learn more about the origin and the steps involved in the development of B cell lymphomas.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Clinical Investigator Award (CIA) (K08)
Project #
5K08CA001005-02
Application #
3079466
Study Section
(SRC)
Project Start
1985-07-01
Project End
1988-06-30
Budget Start
1986-07-01
Budget End
1987-06-30
Support Year
2
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Type
Schools of Medicine
DUNS #
004514360
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Bertoli, L F; Kubagawa, H; Borzillo, G V et al. (1988) Bone marrow origin of a B-cell lymphoma. Blood 72:94-101
Borzillo, G V; Cooper, M D; Bertoli, L F et al. (1988) Lineage and stage specificity of isotype switching in humans. J Immunol 141:3625-33
Bertoli, L F; Burrows, P D (1988) Normal B-lineage cells: their differentiation and identification. Clin Lab Med 8:15-30
Barton, J C; Herrera, G A; Galla, J H et al. (1987) Acute cryoglobulinemic renal failure after intravenous infusion of gamma globulin. Am J Med 82:624-9
Kubagawa, H; Bertoli, L F; Barton, J C et al. (1987) Analysis of paraprotein transport into the saliva by using anti-idiotype antibodies. J Immunol 138:435-9
Kiyotaki, M; Cooper, M D; Bertoli, L F et al. (1987) Monoclonal anti-Id antibodies react with varying proportions of human B lineage cells. J Immunol 138:4150-8