Modulation of anti‐idiotypic immune response by immunization with the autologous M‐component protein in multiple myeloma patients

Multiple myeloma is characterized by a proliferation of clonal B lymphocytes and plasma cells. The idiotypic structure of clonal immunoglobulin (Ig) expressed on the tumour B‐cell surface can be regarded as a tumour‐specific antigen and, as such, a potential target for anti‐idiotypic T and B cells in an immune regulation of the tumour‐cell clone. Active immunization using the autologous monoclonal Ig as a ‘vaccine’ was shown to induce tumour‐specific immunity in murine B‐cell tumours and in human B‐cell lymphoma. With the aim to induce or amplify an anti‐idiotypic response in multiple myeloma, five stage I–III patients were repeatedly immunized with the autologous monoclonal IgG. Induction of idiotype‐specific cellular immunity was analysed in vitro by an enzyme‐linked immunospot assay (interferon‐γ and interleukin‐4 secreting cells). B cells secreting anti‐idiotypic IgM antibodies were also analysed. An anti‐idiotypic T‐cell response was amplified 1.9–5‐fold in three of the five patients during immunization. The number of B cells secreting anti‐idiotypic antibodies also increased in these three patients. In two of the patients induction of idiotype‐specific immunity was associated with a gradual decrease of blood CD19 + B cells. The induced T‐cell response was eliminated during repeated immunization. Further studies are warranted to optimize the immunization schedule in order to achieve a long‐lasting T‐cell immunity against idiotypic determinants on the tumour clone. A role for immunity in controlling the tumour clone remains to be established.