转录因子T-bet、GATA-3、FoxP3及CD4~＋CD25~＋调节性T细胞在儿童过敏性紫癜发病机制中的作用  被引量：7

作　　者：王强[1] 任淑红[1] 董巍[2] 旁俊[2] 

机构地区：[1]四川省人民医院儿科 [2]四川省人民医院,临床医学中心实验室,四川成都610072

出　　处：《中国实验血液学杂志》2012年第1期133-136,共4页Journal of Experimental Hematology

基　　金：四川省卫生厅科研课题(编号303005002209044)

摘　　要：本研究旨在探讨转录因子T-bet、GATA-3和CD4+CD25+调节性T细胞及其转录因子FoxP3在儿童过敏性紫癜(HSP)发病机制中的作用。2009年2月-2010年2月在本院收治的46例急性期HSP患儿(HSP组)及30例健康对照儿童(对照组)纳入研究。采用SYBR GreenⅠ实时荧光定量PCR方法检测外周血单个核细胞T-bet、GATA-3及FoxP3 mRNA的表达。运用流式细胞术检测外周血中T淋巴细胞亚群CD4+CD25+的表达。结果表明,HSP组患儿GATA-3 mRNA相对表达水平(964.30±655.18)显著高于对照组儿童GATA-3 mRNA相对表达水平(78.09±57.20,P<0.01)。HSP组患儿T-bet mRNA(53.98±35.79)、FoxP3 mRNA(32.17±23.04)和CD4+CD25+(5.34±2.51)相对表达水平低于对照组儿童T-bet mRNA(181.56±96.90)、FoxP3 mRNA(147.91±99.15)和CD4+CD25+(7.85±1.97)相对表达水平(P<0.01)。结论:HSP患儿急性期存在Th1特异性转录因子T-betmRNA表达下调,Th2特异性转录因子GATA-3 mRNA表达上调。HSP患儿急性期存在CD4+CD25+调节性T细胞及其特异性转录因子FoxP3 mRNA表达下调,调节性T细胞的减少及由此引发的免疫抑制效应不足可能是HSP急性期免疫失衡的重要原因之一。本研究为从调节性T细胞及其调控的分子机制角度进一步阐明儿童HSP的发病机制提供了实验依据。The aim of this study was to investigate the effects of transcription factors T-bet, GATA-3 in the pathogenesis of Hench-Schonlein purpura （HSP） in children, the relationship between CD4 ＋ CD25 ＋ regulatory T cells, transcription factor FoxP3 and the development of child HSP, and the molecular mechanisms of Thl/Th2 imbalance of child HSP at acute phase, so as to may provide a new approach and strategy for the treatment of HSP at the molecular levels. The expression of T-bet, GATA-3 and FoxP3 mRNA were detected by real time PCR using SYBR Green I in 46 patients with HSP at acute phase and 30 healthy childran as controls. The expression of T lymphocyte subsets CD4 ＋ CD25 ＋ in peripheral blood mononuclear cells was detected by flow cytometry. The results showed that the relative level of GATA- 3 mRNA in peripheral blood mononuclear cells of patients with lISP was significantly higher than those of the control group （964.30 ±655.18 vs 78.09 ±57.20, P 〈0.01 ）. The relative level of T-bet mRNA in peripheral blood mononuclear cells of patients with HSP was lower than those of the control group （53.98 ±35.79 vs 181.56 ± 96.90, P 〈0.01 ）. The expression level of FoxP3 mRNA with lISP was lower than that of the control group （32.17 ±23.04 vs 147.91±99.15, P 〈 0.01 ）. The result of CD4 ＋ CD25 ＋ Treg with HSP was lower than those of the control group （5.34 ±2.51 ） % vs （7. 85 ± 1.97 ）%, P 〈 0.01 ）1. It is concluded that Thl/Th2 imbalance exists in acute phase of child HSP, especially predominant activation of Th2, which correlates with the abnormal expression of transcription factor T-bet and GATA-3 mRNA. At acute phase of child HSP, the expression of CD4 ＋ CD25＋ Treg and its special transcription factor FoxP3 mRNA are down-regulated. Treg cells decreases, which indicates that insufficient immunosuppressive effects resulting fromthe reduction of Treg cells may be one of the important reason in the immune imbalance of HSP acute phase. This study provides experimental e

关 键 词：T-BET GATA-3 FOXP3 CD4+CD25+调节性T细胞 儿童过敏性紫癜 

分 类 号：R554.6[医药卫生—血液循环系统疾病]