AUTOANTIBODY-ASSOCIATED CROSS-REACTIVE IDIOTYPES EXPRESSED AT HIGH-FREQUENCY IN CHRONIC LYMPHOCYTIC-LEUKEMIA RELATIVE TO B-CELL LYMPHOMAS OF FOLLICULAR CENTER CELL ORIGIN
- 1 August 1988
- journal article
- research article
- Vol. 72 (2) , 422-428
Abstract
Using murine monoclonal antibodies (MoAbs) specific for immunoglobulin (Ig) cross-reactive idiotypes (CRI), we performed immunohistochemical analyses on frozen tissue sections and cytocentrifuge preparations of Ig-expressing malignant cells from patients with chronic lymphocytic leukemia (CLL) and B-cell non-Hodgkin''s lymphomas (NHL) of follicular center cell origin. Twenty percent (4/20) of the Ig .kappa. light chain-expressing CLL cells reacted with 17.109, a MoAb against a major CRI on human IgM autoantibodies that is encoded by a conserved Ig variable-region gene (V gene) of the V.kappa.IIIb sub-subgroup. Another MoAb specific for V.kappa.IIIb framework determinant(s) reacted exclusively with all the 17.109-reactive CLL cells. Only one of 20 .kappa. light-chain-expressing CLL cells reacted with 6B6.6, a monoclonal antibody specific for a CRI commonly found on rheumatoid factor (RF) paraproteins with light-chain variable regions of the V.kappa.IIIa sub-subgroup. Finally, a greater than 20% (8/34) of all CLL reacted with G6, a MoAb specific for an Ig heavy chain-associated CRI present on several RF paraproteins. In contrast, these CRIs were expressed at significantly lower frequencies in NHL of follicular center cell origin. Only one of 30 NHL expressing .kappa. light chains reacted with the 17.109 MoAb. Also, in contrast to the concordance between the 17.109-CRI and V.kappa.IIIb framework determinant(s) in CLL, two lymphomas in addition to the 17.109-reactive lymphoma were recognized by the anti-V.kappa.IIIb framework MoAb. None of the NHL reacted with either the 6B6.6 or the G6 MoAbs. These results are the first to demonstrate that CLL and NHL differ with respect to the expression of autoantibody-associated CRIs. The data support the notion that NHL of follicular center cell origin differs from CLL in its utilization and/or somatic mutation of Ig variable-region genes. The physiological and immunotherapeutic implications of these findings are discussed.This publication has 26 references indexed in Scilit:
- Human B cell development. II. Subpopulations in the human fetus.The Journal of Immunology, 1985
- Organization and evolution of a gene cluster for human immunoglobulin variable regions of the kappa typeJournal of Molecular Biology, 1984
- An idiotype-specific helper population that bears immunoglobulin, Ia, and Lyt-1 determinants.The Journal of Experimental Medicine, 1984
- MONOCLONAL-ANTIBODIES REACTIVE WITH IDIOTYPIC AND VARIABLE-REGION SPECIFIC DETERMINANTS ON HUMAN-IMMUNOGLOBULINS1984
- Immunoglobulin isotype expression of normal pre-B cells as determined by immunofluorescenceJournal of Clinical Immunology, 1982
- Structural characterization of the human T cell surface antigen (p67) isolated from normal and neoplastic lymphocytes.The Journal of Immunology, 1982
- Infrequent normal B lymphocytes express features of B-chronic lymphocytic leukemia.The Journal of Experimental Medicine, 1982
- A new human T-cell differentiation antigen: Unexpected expression on chronic lymphocytic leukemia cellsImmunogenetics, 1980
- A monoclonal antibody blocking human T cell functionEuropean Journal of Immunology, 1980
- Human T cell antigens defined by monoclonal antibodies: the 65,000-dalton antigen of T cells (T65) is also found on chronic lymphocytic leukemia cells bearing surface immunoglobulin.The Journal of Immunology, 1980