IL-2 Inhibited the Generation of CD4+ Memory T Cells

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作者
Hongjuan Lu
Jie Chen
Xuefeng Nie
Cong Liu
Weimin Sun
机构
[1] Second Military Medical University,Department of Immunology, National Key Laboratory of Medical Immunology and Institute of Immunology
[2] Second Military Medical University,Rheumatism Immunity Department, Changzheng Hospital
[3] 117th Hospital of PLA,Department of Ophthalmology
[4] Chengdu Military Region,Department of Centre for Disease Prevention and Control
[5] Second Military Medical University,Department of Radiation Medicine, Faculty of Naval Medicine
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IL-2; CD4; memory T cell; IL-15; PI3K/AKT;
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摘要
The survival of T cells at different stages of development is dependent on extrinsic signals. IL-7 is necessary for the development of memory T cells. IL-7 could induce and maintain the differentiation, survival, and proliferation of CD4+ memory T cells, and the roles of IL-2 and IL-15 in the generation of CD4+ memory T cells were still unclear. A CD4+ memory T cells in vitro generated system by adding IL-7. The phenotype of CD4+ memory T cells was identified by FACS. The cells proliferation was analyzed by CFSE staining. The involved signal pathways were analyzed by Western blot. We found that IL-2, not IL-15, could inhibit CD4+ memory T cells generation. Western blot showed that IL-7 up-regulated the P-STAT5A expression and down-regulated Bax expression, IL-2 reduced the effect of IL-7. Besides, IL-2-combined IL-7 up-regulated the P-AKT and Foxo3a expression a little. In conclusion, our data revealed the inhibitory role of IL-2 in CD4+ memory T cells generation and indicated that PI3K/AKT signal pathway was involved.
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页码:1705 / 1711
页数:6
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