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Binding Sites of Interleukin-3-Mimetic Monoclonal Autoantibodies Derived from a MRL/lpr Mouse

 

作者: SugawaraMinoru,   MiyajimaAtsushi,   TanakaHiroshi,   TezukaEmiko,   HattoriChigusa,   OhtaYumiko,  

 

期刊: Autoimmunity  (Taylor Available online 1990)
卷期: Volume 6, issue 1-2  

页码: 61-70

 

ISSN:0891-6934

 

年代: 1990

 

DOI:10.3109/08916939008993370

 

出版商: Taylor&Francis

 

关键词: Monoclonal autoantibody;IL-3-like activity;anti-IL-3 antibody;Anti-IL-3 receptor antibody

 

数据来源: Taylor

 

摘要:

MRL/lpr mouse-derived interleukin-3 (IL-3)-mimetic monoclonal antibodies were examined for their binding sites. One of these five antibodies (B10, F8, F9, F12, H 11), F9 interacted with the IL-3 receptor, as if it were an anti-idiotypic antibody; the IL-3-mimetic activity of F9 was blocked by a neutralizing rat monoclonal anti-IL-3 antibody. IL-3 mRNA was not detected in hybridoma F9, as analyzed by the SI protection assay, Thus, the activity neutralized by the rat antibody is of the F9 antibody itself but not the IL-3 type. Such blocking was not observed with the IL-3-mimetic activity of the other MRL/lpr-derived monoclonal antibodies. On the other hand, the binding of all these monoclonal antibodies to IL-3-depen-dent cells was inhibited by each other andvice versa, as analyzed by two-color flow cytometry. This indicates that the binding sites of the five monoclonal antibodies are located so close to each other that the binding of one would interfere with the binding of any one of the others (since the binding experiment was done on ice, it is unlikely that the inhibition is due to down-modulation of the receptors). Taken together the results obtained by the enzyme digestion study, we discussed that all five IL-3-mimetic monoclonal antibodies are directed to the IL-3 receptor, but only F9 binds to the portion directly responsible for the binding of IL-3 and the other antibodies (B10, F8, F12, H11) bind to different portions, respectively, which are adjacent or overlapping to the binding site of F9.

 

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