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Differences Between Human Hybridoma Platelet-Binding Antibodies Derived from Systemic Lupus Erythematosus Patients and Normal Individuals

 

作者: HuaQiang,   RauchJoyce,  

 

期刊: Autoimmunity  (Taylor Available online 1990)
卷期: Volume 5, issue 3  

页码: 151-167

 

ISSN:0891-6934

 

年代: 1990

 

DOI:10.3109/08916939009002974

 

出版商: Taylor&Francis

 

关键词: SLE;normal;hybridoma autoantibodies;platelet-binding;anti-phospholipid;polyspecificity

 

数据来源: Taylor

 

摘要:

The binding and functional activities of platelet-binding hybridoma autoantibodies from SLE patients were compared with those derived from normal individuals. Twenty-nine SLE-derived hybridoma antibodies and 20 normal-derived hybridoma antibodies were analyzed for binding to glutaraldehyde fixed platelets, dDNA and phospholipids, and for lupus anticoagulant activity. Twenty-four of the 29 SLE-derived antibodies and 9 of the 20 normal-derived antibodies showed one or more activities in these assays. Of the 24 SLE-derived antibodies, 8 (33.3%) were reactive in only one assay (monospecific), while the other 16 (66.7%) had more than one of these activities (polyspecific). In contrast, none (0%) of the 9 normal-derived antibodies with known activities were monospecific, while all 9 (100%) showed polyspecificity. Statistical analyses demonstrated that there was no correlation of anti-DNA activity with anti-platelet and most anti-phospholipid activities for the SLE-derived antibodies, and strong positive correlations between these reactivities for the normal-derived antibodies. Similarly, differences were observed in Western blotting analyses; SLE-derived antibodies bound more specifically to individual platelet proteins than normal-derived antibodies. Moreover, in chromium-51 release assays, all of the SLE-derived platelet-binding antibodies were cytotoxic to platelets, while none of the normal-derived platelet-binding antibodies showed significant cytotoxicity. Our results suggest that hybridoma platelet-binding autoantibodies derived from SLE patients exhibit greater antigen specificity and functional activity than similar antibodies derived from normal individuals.

 

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