技术资料
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Pospori C et al. (JUN 2011) Blood 117 25 6813--24
Specificity for the tumor-associated self-antigen WT1 drives the development of fully functional memory T cells in the absence of vaccination.
Recently,vaccines against the Wilms Tumor antigen 1 (WT1) have been tested in cancer patients. However,it is currently not known whether physiologic levels of WT1 expression in stem and progenitor cells of normal tissue result in the deletion or tolerance induction of WT1-specific T cells. Here,we used an human leukocyte antigen-transgenic murine model to study the fate of human leukocyte antigen class-I restricted,WT1-specific T cells in the thymus and in the periphery. Thymocytes expressing a WT1-specific T-cell receptor derived from high avidity human CD8 T cells were positively selected into the single-positive CD8 population. In the periphery,T cells specific for the WT1 antigen differentiated into CD44-high memory phenotype cells,whereas T cells specific for a non-self-viral antigen retained a CD44(low) naive phenotype. Only the WT1-specific T cells,but not the virus-specific T cells,displayed rapid antigen-specific effector function without prior vaccination. Despite long-term persistence of WT1-specific memory T cells,the animals did not develop autoimmunity,and the function of hematopoietic stem and progenitor cells was unimpaired. This is the first demonstration that specificity for a tumor-associated self-antigen may drive differentiation of functionally competent memory T cells. View Publication产品号#:
09600
09650
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StemSpan™ SFEM
StemSpan™ SFEM
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- B 细胞 235
- CD4+ T细胞 147
- CD8+ T细胞 115
- CHO细胞 15
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- PSC衍生 32
- T 细胞 444
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- 中胚层 3
- 乳腺细胞 97
- 先天性淋巴细胞 32
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- 其他细胞系 10
- 内皮细胞 8
- 内胚层 2
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- 单个核细胞 96
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- 浆细胞 19
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- 癌细胞及细胞系 150
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- 白血病/淋巴瘤细胞 15
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- 真皮细胞 3
- 神经干/祖细胞 467
- 神经细胞 8
- 粒细胞及其亚群 95
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- 造血细胞 1
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- PSC衍生心肌细胞 32
- PSC衍生神经细胞 140
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- PSC衍生造血干细胞 45
- PSC衍生间充质细胞 32
- 其他T细胞亚型 32
- 呼吸道细胞 101
- 多巴胺能神经元 7
- 小鼠胚胎成纤维细胞 1
- 神经元 203
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