首页   按字顺浏览 期刊浏览 卷期浏览 Antigen-Specific Tolerance as a Therapy for Experimental Autoimmune Encephalomyelitis
Antigen-Specific Tolerance as a Therapy for Experimental Autoimmune Encephalomyelitis

 

作者: MillerStephen D.,   TanL. J.,   PopeLouise,   McRaeBradford L.,   KarpusWilliam J.,  

 

期刊: International Reviews of Immunology  (Taylor Available online 1992)
卷期: Volume 9, issue 3  

页码: 203-222

 

ISSN:0883-0185

 

年代: 1992

 

DOI:10.3109/08830189209061791

 

出版商: Taylor&Francis

 

关键词: autoimmunity;experimental autoimmune encephalomyeliti;immune tolerance;myelin basic protei;proteolipid protein

 

数据来源: Taylor

 

摘要:

The effects of neuroantigen-specific tolerance on the induction and effector stages of EAE were examined. Tolerance induced by the i.v. injection of syngeneic splenocytes coupled with purified neuroantigens or encephalitogenic peptides of MBP and PLP using ethylene carbodiimide was extremely effective in both prevention and treatment of acute and relapsing forms of EAE in Lewis rats and SJL/J mice. The unresponsiveness is rapidly-induced, dose-dependent, long-lasting, efficient, MHC class II-restricted, and exquisitely antigen-specific. This procedure targets only effector cells bearing clonotypic receptors specific for the autoantigen/ autoepitope and thus does not depend upon the autoimmune response being dominated by a restricted T cell repertoire. Moreover, it does not require that the response to the autoantigen be dominated by recognition of a specific epitope(s) within a particular autoantigen, or even the identification of the specific autoantigen. The results also demonstrate the usefulness of peripheral tolerance induced by antigen-coupled syngeneic splenocytes for identifying the fine specificity of autoimmune T cell responses which appear to change during the progression of relapsing EAE. Thus, this technique offers major advantages over many other currently employed immunoregula-tory strategies and is therefore relevant for establishment of therapeutic protocols for the antigen-specific treatment of human T cell-dependent autoimmune disorders.

 

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