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Reversible HLA multimers (Streptamers) for the isolation of human cytotoxic T lymphocytes functionally active against tumor- and virus-derived antigens
Authors:Neudorfer Julia  Schmidt Burkhard  Huster Katharina M  Anderl Florian  Schiemann Matthias  Holzapfel Gerd  Schmidt Thomas  Germeroth Lothar  Wagner Hermann  Peschel Christian  Busch Dirk H  Bernhard Helga
Affiliation:

aDepartment of Hematology/Oncology, Klinikum rechts der Isar, Technical University of Munich, Germany

bDepartment of Microbiology/Immunology, Klinikum rechts der Isar, Technical University of Munich, Germany

cIBA GmbH, Göttingen, Germany

dStage Pharmaceuticals GmbH, Göttingen, Germany

eClinical Cooperation Group ‘Antigen-Specific Immunotherapy’, GSF - Institute of Health and Environment and Technical University of Munich, Germany

Abstract:
The development of MHC/peptide multimers has facilitated the visualization and purification of antigen-specific T cells. However, the persistence of multimers leads to prolonged T cell receptor signaling and subsequently to altered T-cell function. We have recently developed a new type of MHC/peptide multimers, which can be dissociated from the T cell. Herein, we have generated and tested for the first time reversible HLA/peptide multimers, termed Streptamers, for the isolation of human T cells. The Streptamer technique demonstrates the specificity and sensitivity of conventional HLA/peptide tetramers with regards to the sorting of human T lymphocytes. This is shown for T cells directed against immunogenic peptides derived from viral and tumor-associated antigens. We show that antigen-specific cytotoxic T cells remain functionally active following Streptamer dissociation, whereas lytic function and proliferation of the T cells is impaired in the presence of conventional tetramers. These novel HLA/peptide Streptamer reagents allow the isolation of antigen-specific T cells with preserved function and, therefore, facilitate the development of adoptive T cell transfer regimens for the treatment of patients with cancer or infectious diseases.
Keywords:Human   Cytotoxic T cells   MHC   Tumor immunity   T cell receptors
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