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Blood, 15 November 2007, Vol. 110, No. 10, pp. 3564-3572. Prepublished online as a Blood First Edition Paper on July 27, 2007; DOI 10.1182/blood-2007-02-075010.
GENE THERAPY Selecting highly affine and well-expressed TCRs for gene therapy of melanoma1 Department of Immunology, the Netherlands Cancer Institute (NKI), Amsterdam, the Netherlands; 2 Department of Immunohematology and Blood Transfusion, Leiden University Medical Center, Leiden, the Netherlands; 3 Division of Clinical Onco-Immunology, Ludwig Institute for Cancer Research, Lausanne, Switzerland; and 4 Surgery Branch, National Cancer Institute, National Institutes of Health (NIH), Bethesda, MD A recent phase 1 trial has demonstrated that the generation of tumor-reactive T lymphocytes by transfer of specific T-cell receptor (TCR) genes into autologous lymphocytes is feasible. However, compared with results obtained by infusion of tumor-infiltrating lymphocytes, the response rate observed in this first TCR gene therapy trial is low. One strategy that is likely to enhance the success rate of TCR gene therapy is the use of tumor-reactive TCRs with a higher capacity for tumor cell recognition. We therefore sought to develop standardized procedures for the selection of well-expressed, high-affinity, and safe human TCRs. Here we show that TCR surface expression can be improved by modification of TCR alpha and beta sequences and that such improvement has a marked effect on the in vivo function of TCR gene-modified T cells. From a panel of human, melanoma-reactive TCRs we subsequently selected the TCR with the highest affinity. Furthermore, a generally applicable assay was used to assess the lack of alloreactivity of this TCR against a large series of common human leukocyte antigen alleles. The procedures described in this study should be of general value for the selection of well- and stably expressed, high-affinity, and safe human TCRs for subsequent clinical testing.
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