AI Article Synopsis
- Monoclonal anti-idiotype antibodies were tested in a clinical trial for treating B lymphocytic malignancies, resulting in tumor regression in some patients.
- Characteristics of the antibodies and tumors were analyzed, showing that factors like the antibody isotype and avidity were not predictive of clinical outcomes, while reactivity with specific tumor components had some correlation.
- The effectiveness of the treatment varied; in one case, the antibody directly impacted tumor cells, while in others, the response was linked to the presence of host immune cells, particularly mature T lymphocytes, suggesting that existing host-tumor interactions play a crucial role in treatment efficacy.
Article Abstract
Monoclonal anti-idiotype antibodies can be made which are exquisitely specific for B lymphocytic malignancies. We have conducted a clinical trial in which some patients' tumors regressed after infusion of such antibodies. Here, we evaluated characteristics of the antibodies, the tumors, and the patients to determine which features best correlated with the clinical response. Neither the isotype of the murine antibodies, nor their avidity were predictive of clinical outcome. The specific epitope to which the antibodies bound was characterized by immunochemical techniques. Reactivity with a heavy-light chain combinatorial determinant correlated somewhat with clinical effect. Variations in the characteristics of the individual tumors such as antigen sites per cell and ability to modulate the surface immunoglobulin were not predictive of response. In one patient with prolymphocytic leukemia the anti-idiotype antibody had a direct antiproliferative effect on tumor cells in vitro. This patient's tumor response was explainable by such a direct mechanism. In the other patients, who had lymphomas, therapeutic outcome correlated with the number of host nontumor cells infiltrating the tumor. The vast majority of these nontumor cells were mature T lymphocytes of the Leu 4, Leu 3 (T3, T4) phenotype. Thus, a preexistent host-tumor interaction seems to be important in the in vivo effect of anti-idiotype antibodies in B cell tumors.
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