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公开(公告)号:US11214627B2
公开(公告)日:2022-01-04
申请号:US16307454
申请日:2017-06-08
Applicant: UCB BIOPHARMA SRL
Inventor: Ralph Adams , Thomas Allen Ceska , Anna Marie Davies , Alistair James Henry , Xiaofeng Liu , James Michael McDonnell , Brian John Sutton , Marta Katarzyna Westwood
IPC: C07K16/42 , C07K16/28 , C07K14/735 , A61P37/08
Abstract: The present invention relates to the area of improved anti-IgE antibodies and antigen binding agents, and compositions thereof, which target IgE, for instance: for use in treating disorders caused by IgE (such as allergic responses, or certain autoimmune responses); and, in particular, disorders caused by the interaction of IgE with the FcεRI receptor. In particular, this invention relates to improved anti-IgE antibodies and antigen binding agents related to novel mutants of omalizumab (Xolair®). The improved anti-IgE antibodies and antigen binding agents of the invention may have improved affinity for IgE and/or an improved interaction with the Cε2 domain of IgE and/or an improved modified epitope on IgE (for instance further involving the Cε2 domain of IgE) and/or the ability to disassociate IgE from the FcεRI receptor for instance at pharmaceutically-relevant concentrations. In one aspect, improved or novel treatments for IgE mediated disorders are disclosed in which IgE is targeted (for instance free IgE and/or IgE complexed with the FcεRI receptor).
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公开(公告)号:US12054559B2
公开(公告)日:2024-08-06
申请号:US17541932
申请日:2021-12-03
Applicant: UCB BIOPHARMA SRL
Inventor: Ralph Adams , Thomas Allen Ceska , Anna Marie Davies , Alistair James Henry , Xiaofeng Liu , James Michael McDonnell , Brian John Sutton , Marta Katarzyna Westwood
IPC: C07K16/42 , A61P37/08 , C07K14/735 , C07K16/28
CPC classification number: C07K16/4291 , A61P37/08 , C07K14/70535 , C07K16/2851 , C07K2317/565 , C07K2317/92
Abstract: The present invention relates to the area of improved anti-IgE antibodies and antigen binding agents, and compositions thereof, which target IgE, for instance: for use in treating disorders caused by IgE (such as allergic responses, or certain autoimmune responses); and, in particular, disorders caused by the interaction of IgE with the FcεRI receptor. In particular, this invention relates to improved anti-IgE antibodies and antigen binding agents related to novel mutants of omalizumab (Xolair®). The improved anti-IgE antibodies and antigen binding agents of the invention may have improved affinity for IgE and/or an improved interaction with the Cε2 domain of IgE and/or an improved modified epitope on IgE (for instance further involving the Cε2 domain of IgE) and/or the ability to disassociate IgE from the FcεRI receptor for instance at pharmaceutically-relevant concentrations. In one aspect, improved or novel treatments for IgE mediated disorders are disclosed in which IgE is targeted (for instance free IgE and/or IgE complexed with the FcεRI receptor).
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