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Anti-tumor effects of endogenous prostate cancer-specific CD8 T cells in a murine TCR transgenic model

机译:内源性前列腺癌特异性CD8 T细胞在小鼠TCR转基因模型中的抗肿瘤作用

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Background: The CD8 T-cell response to prostate and other cancers is often functionally diminished or absent. This may occur via deletion of tumor-specific T cells, through acquisition of an anergic phenotype, or via active suppression mediated by another population of cells. METHODS We used a double transgenic model in which mice express CD8 T cells specific for a prostate/prostate cancer antigen to study the response of CD8 T cells to evolving autochronous prostate tumors in TRAMP mice. CD8 T cells were analyzed for functionality by measuring IFN-? production via flow cytometry and via an in vivo CTL killing assay. In addition, pathological scoring of the prostates of the double transgenic mice was compared to scoring of tumor burden prostates of ProTRAMP mice. Results: Tumor-specific CD8 T cells were not grossly deleted in these animals, but evidenced a clearly non-functional phenotype. Interestingly, full lytic function was rapidly recovered upon removal from tumor-bearing mice. Conclusions: These data indicate a role for continuous antigen exposure in the maintenance of tumor-specific CD8 T-cell tolerance to prostate cancer.
机译:背景:CD8 T细胞对前列腺癌和其他癌症的反应通常在功能上减弱或缺失。这可能是由于肿瘤特异性T细胞的缺失,无性表型的获得或另一细胞群介导的活性抑制引起的。方法我们使用双转基因模型,其中小鼠表达对前列腺/前列腺癌抗原具有特异性的CD8 T细胞,以研究CD8 T细胞对TRAMP小鼠中不断发展的自发性前列腺肿瘤的反应。通过测量IFN-γ来分析CD8 T细胞的功能。通过流式细胞术和体内CTL杀伤测定法进行生产。另外,将双转基因小鼠的前列腺的病理评分与ProTRAMP小鼠的肿瘤负荷前列腺的评分进行了比较。结果:这些动物中的肿瘤特异性CD8 T细胞并未完全缺失,但表现出明显的无功能表型。有趣的是,从荷瘤小鼠中取出后,其全部溶解功能迅速恢复。结论:这些数据表明连续抗原暴露在维持肿瘤特异性CD8 T细胞对前列腺癌耐受性中的作用。

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