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用CTLA4Ig和致脑炎肽对抗原呈递细胞进行体外处理可预防Lewis大鼠的实验性自身免疫性脑脊髓炎。

Ex vivo treatment of antigen-presenting cells with CTLA4Ig and encephalitogenic peptide prevents experimental autoimmune encephalomyelitis in the Lewis rat.

作者信息

Khoury S J, Gallon L, Verburg R R, Chandraker A, Peach R, Linsley P S, Turka L A, Hancock W W, Sayegh M H

机构信息

Brigham and Women's Hospital, Harvard Medical School, Boston, MA 02115, USA.

出版信息

J Immunol. 1996 Oct 15;157(8):3700-5.

PMID:8871673
Abstract

We used a novel approach to study the role of CD28-B7 T cell costimulatory blockade in experimental autoimmune encephalomyelitis (EAE) in the Lewis rat model. APCs were incubated in vitro with CTLA4Ig and the encephalitogenic peptide p71-90 of myelin basic protein. Systemic injection of APCs treated ex vivo with p71-90 and CTLA4Ig before immunization protected animals from clinical EAE. Systemic injection of APCs treated with CTLA4Ig alone, CTLA4Ig and control peptide, peptide alone, or peptide and control Ig was not protective. Injection of APCs treated ex vivo with CTLA4Ig and p71-90 on the day of immunization was also protective, but delaying the injection till day 7 after immunization impaired the protective effect. Immunohistologically, protected animals had decreased inflammatory responses, with inhibition of Th1 and sparing of Th2 cytokines in the brain. Preincubation of APCs with p71-90 and a mutant form of CTLA4Ig that binds only B7-1 also protected animals from developing EAE. These results suggest that ex vivo blockade of CD28-B7-1 leads to the generation of regulatory cells, presumably Th2, which inhibit the generation or priming of encephalitogenic T cells and suppress the autoimmune response to the specific Ag in vivo. These observations have therapeutic implications for autoimmune diseases and transplantation.

摘要

我们采用了一种新方法来研究CD28 - B7共刺激阻断在Lewis大鼠模型实验性自身免疫性脑脊髓炎(EAE)中的作用。将抗原呈递细胞(APCs)与CTLA4Ig以及髓鞘碱性蛋白的致脑炎性肽p71 - 90在体外共同孵育。在免疫前全身注射经p71 - 90和CTLA4Ig体外处理的APCs可保护动物免受临床EAE的侵害。全身注射单独用CTLA4Ig处理的APCs、CTLA4Ig与对照肽、单独的肽或肽与对照Ig均无保护作用。在免疫当天注射经CTLA4Ig和p71 - 90体外处理的APCs也具有保护作用,但将注射推迟至免疫后第7天会削弱保护效果。免疫组织学检查显示,受保护的动物炎症反应减弱,大脑中Th1细胞因子受到抑制,Th2细胞因子得以保留。将APCs与p71 - 90以及仅结合B7 - 1的CTLA4Ig突变体形式预孵育也可保护动物不发生EAE。这些结果表明,体外阻断CD28 - B7 - 1会导致调节性细胞(可能是Th2细胞)的产生,这些调节性细胞可抑制致脑炎性T细胞的产生或致敏,并在体内抑制对特定抗原的自身免疫反应。这些观察结果对自身免疫性疾病和移植具有治疗意义。

相似文献

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Ex vivo treatment of antigen-presenting cells with CTLA4Ig and encephalitogenic peptide prevents experimental autoimmune encephalomyelitis in the Lewis rat.用CTLA4Ig和致脑炎肽对抗原呈递细胞进行体外处理可预防Lewis大鼠的实验性自身免疫性脑脊髓炎。
J Immunol. 1996 Oct 15;157(8):3700-5.
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