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1型糖尿病与脾脏CD4^+CD25^+调节性T细胞及相关基因Foxp3表达的关系 被引量:9

Relationship of type 1 diabetes mellitus with CD4^+CD25^+regulatory T cells and expression of its related gene Foxp3
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摘要 目的:研究链脲佐菌素(streptozotocin,STZ)诱导糖尿病小鼠发病中CD4+CD25+调节性T细胞(regulatoryTcell,Tr)及相关基因Foxp3表达的变化,从而探讨CD4+CD25+Tr在自身免疫耐受中的作用。方法:实验选用健康昆明小鼠60只,将60只小鼠随机分对照组(n=20)和模型组(n=40)。模型组给与腹腔注射6g/LSTZ溶液,60mg/(kg·d),连续5d;对照组给予枸橼酸钠缓冲液0.2mL/d腹腔注射,连续5d。流式细胞仪检测脾脏CD4+和CD4+CD25+Tr细胞数量的变化,RT-PCR检测脾小鼠脾脏细胞中CD4+CD25+Tr细胞相关基因Foxp3mRNA的表达。结果:模型组血糖和抗胰岛素抗体水平明显高于对照组(t=0.023,P<0.05;t=0.018,P<0.05);模型组小鼠脾脏CD4+T细胞数量犤(29.69±4.77)%犦明显高于对照组犤(19.60±11.42)%犦(t=0.014,P<0.05),模型组CD4+CD25+Tr/CD4+T比值低于对照组;Foxp3mR-NA水平模型组的表达普遍高于对照组。结论:CD4+CD25+Tr细胞的相对降低,引起外周耐受状态的打破;在STZ破坏胰岛细胞,自身抗原存在的同时,导致了自身免疫糖尿病的发生。 AIM:To investigate the changes of CD4+CD25+regulatory T cells(Tr) in streptozotocin(STZ)-induced diabetic mice, so as to probe into the mechanism of CD4+CD25+Tr in autoimmune tolerance. METHODS:Sixty healthy Kunming mice were randomly divided into control group(n=20) and model group(n=40).Mice in the model group and control group were treated with intraperitoneal injection of STZ(60 mg/kg per day) and sodium citrate buffer(0.2 mL per day) for 5 days successively respectively.The changes of numbers of CD4+Tr and CD4+CD25+Tr were detected with flow cytometer,and the level of Foxp3 mRNA expression of CD4+CD25+Tr in spleen was determined with reverse transcriptase-polymerase chain reaction(RT-PCR). RESULTS:The levels of blood glucose and anti-insulin were obviously higher in the model group than in the control group(t=0.023, P< 0.05;t=0.018,P< 0.05).The number of CD4+Tr in spleen of mice was markedly higher in the model group[(29.69±4.77)%] than in the control group[(19.60±11.42)%](t=0.014,P< 0.05),while the rate of CD4+CD25+Tr/CD4+T was lower and the level of Foxp3 mRNA expression was higher in the model group than in the control group. CONCLUSION:The relative reduce of CD4+CD25+Tr can lead to the breakdown of peripheral autoimmune tolerance.STZ destroys insulin and existence of self-antigen, meanwhile,results in the occurrence of autoimmune diabetes mellitus.
出处 《中国临床康复》 CSCD 北大核心 2005年第7期45-47,共3页 Chinese Journal of Clinical Rehabilitation
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参考文献8

  • 1Jonuleit H, Adema G, Schmitt E. Immune regulation by regulatory T cells: implications for transplantation. Transpl Immunol 2003; 11 (3 - 4): 267 - 76.
  • 2Fontenote JD, Gavin MA, Rudensky AY. Foxp3 programs the development and function of CD4+CD25 + regulatory T cells. Nat. Immunol(on line) 2003; 4(4): 330 -6.
  • 3Yang Z, Chen M, Fialkow LB, et al. The novel anti-inflammatory compound,lisofylline, prevents diabetes in multiple low-dose streptozotocin-treated mice. Pancreas 2003; 26(4): e99 - 104.
  • 4Rabinovitch A. Immuno regulatary and cytokine imbalances in the pathogenesis of IDDM. Diabetes 1994; 43:613 - 9.
  • 5Hori S, Nomura T, Sakaguchi S. Control of regulatory T cell development by the transcription factor Foxp3. Science 2003; 299(5609): 1057 -61.
  • 6Piccinillo CA, Letterio JJ, et al. CD4 +CD25 + regulatory T cells can mediate suppressor function in the absence of transforming growth factor betal production and responsiveness. J Exp Med 2002; 196 (2): 237 - 46.
  • 7Sakaguchi S, Sakaguchi N, Asano M, et al. Immunologic self-tolerance maintained by activated T cells expressing IL-2 receptor alpha-chains (CD25). Breakdown of a single mechanism of a single mechanism of self-tolerance causes various autoimmune diseases. J Immunol 1995; 155 ( 1 ): 1151 - 64.
  • 8Herold KC, Baumann E, Vezys V, et al. Expression and Immune Response to Islet Antigens following Treatment with Low Dose of Streptozotocin in H-2d Mice. J Autoimmun 1997; 10(1): 17 -25.

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