Major histocompatibility complex class I and unique antigen expression by murine tumors that escaped from CD8 super(+) T-cell-dependent surveillance
The rejection of murine UV-induced skin cancers by normal mice is a striking example of powerful immune surveillance of the normal host against malignant cells. In this study, we show that UV-induced regressor tumors regularly grew progressively and killed mice that were depleted of CD8 super(+) T-c...
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| Veröffentlicht in: | Cancer research (Chicago, Ill.) Ill.), 1990-01, Vol.50 (13), p.3851-3858 |
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| creator | Ward, P Koeppen, H K Hurteau, T Rowley, DA Schreiber, H |
| description | The rejection of murine UV-induced skin cancers by normal mice is a striking example of powerful immune surveillance of the normal host against malignant cells. In this study, we show that UV-induced regressor tumors regularly grew progressively and killed mice that were depleted of CD8 super(+) T-cells. Depletion of CD4 super(+) T-cells had no effect, suggesting that CD8 super(+) but not CD4 super(+) T-cells were required for this immune surveillance. To determine whether change in major histocompatibility complex (MHC) class I expression was a frequent event that caused low immunogenicity of tumors or facilitated escape from immune destruction, recently isolated murine tumors of varying degrees of immunogenicity, including highly immunogenic UV-induced regressor, less immunogenic UV-induced progressor, and poorly immunogenic spontaneous progressor tumors, were compared. There was no correlation between the ability of a tumor to grow progressively in a normal immunocompetent host and the level of constitutive class I expression or the level of expression induced in vitro by gamma interferon. (DBO) |
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In this study, we show that UV-induced regressor tumors regularly grew progressively and killed mice that were depleted of CD8 super(+) T-cells. Depletion of CD4 super(+) T-cells had no effect, suggesting that CD8 super(+) but not CD4 super(+) T-cells were required for this immune surveillance. To determine whether change in major histocompatibility complex (MHC) class I expression was a frequent event that caused low immunogenicity of tumors or facilitated escape from immune destruction, recently isolated murine tumors of varying degrees of immunogenicity, including highly immunogenic UV-induced regressor, less immunogenic UV-induced progressor, and poorly immunogenic spontaneous progressor tumors, were compared. There was no correlation between the ability of a tumor to grow progressively in a normal immunocompetent host and the level of constitutive class I expression or the level of expression induced in vitro by gamma interferon. 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In this study, we show that UV-induced regressor tumors regularly grew progressively and killed mice that were depleted of CD8 super(+) T-cells. Depletion of CD4 super(+) T-cells had no effect, suggesting that CD8 super(+) but not CD4 super(+) T-cells were required for this immune surveillance. To determine whether change in major histocompatibility complex (MHC) class I expression was a frequent event that caused low immunogenicity of tumors or facilitated escape from immune destruction, recently isolated murine tumors of varying degrees of immunogenicity, including highly immunogenic UV-induced regressor, less immunogenic UV-induced progressor, and poorly immunogenic spontaneous progressor tumors, were compared. There was no correlation between the ability of a tumor to grow progressively in a normal immunocompetent host and the level of constitutive class I expression or the level of expression induced in vitro by gamma interferon. (DBO)</abstract></addata></record> |
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| ispartof | Cancer research (Chicago, Ill.), 1990-01, Vol.50 (13), p.3851-3858 |
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| language | eng |
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| source | American Association for Cancer Research; EZB-FREE-00999 freely available EZB journals |
| title | Major histocompatibility complex class I and unique antigen expression by murine tumors that escaped from CD8 super(+) T-cell-dependent surveillance |
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