Immunotherapy in multiple myeloma: Id-specific strategies suggested by studies in animal models

被引:0
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作者
Alexandre Corthay
Katrin U. Lundin
Ludvig A. Munthe
Marianne Frøyland
Tobias Gedde-Dahl
Zlatko Dembic
Bjarne Bogen
机构
[1] Rikshospitalet University Hospital,University of Oslo, Institute of Immunology
[2] Rikshospitalet University Hospital,Department of Medicine
[3] Rikshospitalet University Hospital,Institute of Oral Biology
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关键词
Cancer; Idiotype; Immunosurveillance; T cells; Tolerance;
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摘要
Multiple myeloma (MM) cells produce monoclonal immunoglobulin (Ig) which serves as a truly tumor-specific antigen. The tumor-specific antigenic determinants are localized in the variable (V)-regions of the monoclonal Ig and are called idiotopes (Id). We review here the evidence obtained in a T-cell receptor (TCR) transgenic mouse model that Id-specific, MHC class II–restricted CD4+ T cells play a pivotal role in immunosurveillance and eradication of MHC class II-negative MM cells. In brief, monoclonal Ig secreted by MM cells is endocytosed and processed by antigen-presenting cells (APCs) in the tumor. Such tumor-resident dendritic cell APCs in turn present Id peptide on their class II molecules to Id-specific CD4+ T cells which become activated and indirectly kill the MHC class II-negative myeloma cells. However, if the Id-specific CD4+ cells fail to eliminate the MM cells during their initial encounter, the increasing number of tumor cells secretes so much monoclonal Ig that T-cell tolerance to Id is induced. Extending these findings to MM patients, Id-specific immunotherapy should be applied at a time of minimal residual disease and when new Id-specific T cells have been educated in the thymus, like after high-dose chemotherapy and autologous stem cell transplantation.
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页码:759 / 769
页数:10
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