Detection and Induction of CTLs Specific for SYT-SSX-Derived Peptides in HLA-A24+ Patients with Synovial Sarcoma

To investigate the immunogenic property of peptides derived from the synovial sarcoma-specific SYT-SSX fusion gene, we synthesized four peptides according to the binding motif for HLA-A24. The peptides, SS391 (PYGYDQIMPK) and SS393 (GYDQIMPKK), were derived from the breakpoint of SYT-SSX, and SS449a...

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Veröffentlicht in:The Journal of immunology (1950) 2002-08, Vol.169 (3), p.1611-1618
Hauptverfasser: Sato, Yuriko, Nabeta, Yuki, Tsukahara, Tomohide, Hirohashi, Yoshihiko, Syunsui, Rong, Maeda, Akiko, Sahara, Hiroeki, Ikeda, Hideyuki, Torigoe, Toshihiko, Ichimiya, Shingo, Wada, Takuro, Yamashita, Toshihiko, Hiraga, Hiroaki, Kawai, Akira, Ishii, Takeshi, Araki, Nobuhito, Myoui, Akira, Matsumoto, Seiichi, Umeda, Tohru, Ishii, Seiichi, Kawaguchi, Satoshi, Sato, Noriyuki
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Sprache:eng
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Zusammenfassung:To investigate the immunogenic property of peptides derived from the synovial sarcoma-specific SYT-SSX fusion gene, we synthesized four peptides according to the binding motif for HLA-A24. The peptides, SS391 (PYGYDQIMPK) and SS393 (GYDQIMPKK), were derived from the breakpoint of SYT-SSX, and SS449a (AWTHRLRER) and SS449b (AWTHRLRERK) were from the SSX region. These peptides were tested for their reactivity with CTL precursors (CTLps) in 16 synovial sarcoma patients using HLA-A24/SYT-SSX peptide tetramers and also for induction of specific CTLs from four HLA-A24(+) synovial sarcoma patients. Tetramer analysis indicated that the increased CTLp frequency to the SYT-SSX was associated with pulmonary metastasis in synovial sarcoma patients (p < 0.03). CTLs were induced from PBLs of two synovial sarcoma patients using the peptide mixture of SS391 and SS393, which lysed HLA-A24(+) synovial sarcoma cells expressing SYT-SSX as well as the peptide-pulsed target cells in an HLA class I-restricted manner. These findings suggest that aberrantly expressed SYT-SSX gene products have primed SYT-SSX-specific CTLps in vivo and increased their frequency in synovial sarcoma patients. The identification of SYT-SSX peptides may offer an opportunity to design peptide-based immunotherapeutic approaches for HLA-A24(+) patients with synovial sarcoma.
ISSN:0022-1767
1550-6606
DOI:10.4049/jimmunol.169.3.1611