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IL-2通过上调naive CD4+T细胞SOCS-3表达抑制CD4+T细胞的极化和增殖
引用本文:谢彦晖,吴敏,张腾龙,赵金河,王缨,林果为.IL-2通过上调naive CD4+T细胞SOCS-3表达抑制CD4+T细胞的极化和增殖[J].中华微生物学和免疫学杂志,2008,28(7):610-615.
作者姓名:谢彦晖  吴敏  张腾龙  赵金河  王缨  林果为
作者单位:1. 复旦大学附属华山医院血液科,上海,200040
2. 青岛市立医院血液科
3. 复旦大学上海医学院免疫学教研室
基金项目:上海市科委生物医药重大课题科技攻关项目 
摘    要:目的 探讨IL-2预孵育naive CD4+T细胞后,对其极化(polarization)方向和增殖(proliferation)能力的影响.方法 用终浓度为50 U/ml的IL-2分别预孵育DOI 1.10 TCR转基因小鼠和C57BL/6N小鼠naYve CD+T细胞,在不同时间点用荧光实时定量PCR(real-time PCR)检测这两种细胞中SOCS-3(suppressor of cytokine signal-3)表达的变化.预孵育4 h后,洗去IL-2,分别加入卵清白蛋白(OVA)和灭活后的BALB/c脾细胞,在存在细胞因子IL-12或IL-4情况下共培养14 d后,用流式细胞仪检测TH1细胞活化和极化的标志IL-12R β1、IL-12Rβ2,对C57BL/6N小鼠nave CD4+2T细胞的极化中还榆测TH2极化的标志--细胞内IL-4的表达;同时将无IL-2预孵育的作为对照组.结果 IL-2预孵育后这两种鼠naive CD4+T细胞内的SOCS-3表达于6 h达高峰;在SOCS-3表达达高峰后分别给予特异性抗原和同种异基因抗原刺激,其向TH1方向的极化和增殖能力都受到明显的抑制(P<0.05).结论 IL-2预孵育naive CD+T细胞后,可以上调SOCS-3的表达;SOCS-3的上调表达可以抑制naive CD4+T细胞接受特异性抗原和同种异基因抗原刺激后向TH1方向的极化和增殖能力.

关 键 词:白细胞介素(IL)-2  Naive  CD-T淋巴细胞  TH1细胞

The polarization and proliferation of TH1 cells inhibited IL-2 through upregulation of SOCS-3 in naive CD4+T cells
XIE Yan-hui,WU Min,ZHANG Teng-long,ZHAO Jin-he,WANG Ying,LIN Guo-wei.The polarization and proliferation of TH1 cells inhibited IL-2 through upregulation of SOCS-3 in naive CD4+T cells[J].Chinese Journal of Microbiology and Immunology,2008,28(7):610-615.
Authors:XIE Yan-hui  WU Min  ZHANG Teng-long  ZHAO Jin-he  WANG Ying  LIN Guo-wei
Abstract:Objective To explore the polarization and proliferation of naive CD4+TT cells after preincubation with interleukin-2. Methods The expression of suppressor of cytokine signal (SOCS)-3 was detected by the real-time PCR in the naive T lymphocytes of DO11.10 TCR transgenic and C57BL/6N mice after they were preincubated by 50 U/ml of IL-2. The naive CD4+T T lymphocytes preincubated for 4 h by IL-2 were stimulated with ovalbumin (OVA) and inactivated BALB/c spleen cells, respectively. After 14 d, IL-12Rβ1, IL-12β2 and cytoplasm IL-4 (cyIL-4) were detected by flow cytometry. Results SOCS-3 in the naive CD4+T lymphocytes of DO11. 10 TCR transgenic and C57BL/6N mice reached the peak after preincu- bated by IL-2 for 6 h. The polarization to TH1 and the proliferation ability of naive CD4+ T lymphocytes stimulated with specific antigen and allogeneic antigen were inhibited conspicuously during the time of the peak of SOCS-3. Conclusion The expression of SOCS-3 in naive CD4+T lymphocytes can be upregulated by IL-2. The upregulation of SOCS-3 can suppress the polarization to TH1and the proliferation ability of naive CD4+T lymphocytes stimulated by specific antigen and allogeneic antigen.
Keywords:SOCS-3
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