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Non-fastidious,melanoma-specific CD8+ cytotoxic T lymphocytes from choroidal melanoma patients
Authors:Xiu Qing Huang  Malcolm S Mitchell  Peter E Liggett  A Linn Murphree  June Kan-Mitchell
Institution:(1) Department of Pathology, University of Southern California School of Medicine, Los Angeles, California, USA;(2) Department of Medicine, University of Southern California School of Medicine, Los Angeles, California, USA;(3) Department of Ophthalmology, Doheny Eye Institute, University of Southern California School of Medicine, Los Angeles, California, USA;(4) Norris 710, University of Southern California School of Medicine, 2025 Zonal Avenue, 90033 Los Angeles, CA, USA
Abstract:To characterize the anti-melanoma reactivity of CD8+ cytotoxic T lymphocytes (CTL) from choroidal melanoma patients, CTL clones were isolated from the peripheral blood of three patients after mixed lymphocyte/tumor cell culture (MLTC). Clones were derived from lymphocytes stimulated by allogeneic (OCM-1, A24, A28) or autologous (OCM-3, Al, A30) melanoma cells. Their reactivity against a panel of HLA-typed melanoma and nonmelanoma cells was assessed, to determine whether a single CTL clone could recognize and lyse a variety of allogeneic melanoma cell lines. While proportionately more clones derived from autologous MLTC were melanoma-specific than allogeneic MLTC (42% versus 14%), melanoma-specific CTL were recovered from both. Notably, a novel melanoma specificity was identified. These CTL clones were termed non-fastidious because they were capable of lysing melanoma cells with which they had no HLA class I alleles in common. Nonetheless, lysis was mediated by the HLA class I molecule. Since lysis was specific for melanoma cells, these CTL appeared to recognize a shared melanoma peptide(s). Because of their prevalence, we propose that non-fastidious CTL are integral to human anti-melanoma T cell immunity. This reinforces clinical findings that allogeneic melanomas can substitute for autologous tumors in active specific immunotherapy. By circumventing the need for autologous melanoma, it is possible to treat patients after removal of the primary choroidal melanoma in an attempt to prevent metastasis.Supported by USPHS grants EY-09031 and EY-09427, and the Lucy Adams Choroidal Melanoma Research Fund to J. K.-M.
Keywords:Cytotoxic T cell  Clone  Choroidal melanoma  Melanoma-specific  HLA restriction
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