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公开(公告)号:US08093355B2
公开(公告)日:2012-01-10
申请号:US12580112
申请日:2009-10-15
申请人: Rolf E. Kuestner , Zeren Gao , Steven D. Levin , Mark W. Rixon
发明人: Rolf E. Kuestner , Zeren Gao , Steven D. Levin , Mark W. Rixon
CPC分类号: C07K14/7155 , A61K38/00 , A61K2121/00 , C07K14/715 , C07K16/2866 , C07K2317/73 , C07K2317/76 , C07K2319/21 , C07K2319/30 , C07K2319/43
摘要: The present invention relates to blocking, inhibiting, reducing, antagonizing or neutralizing the activity of IL-17F, IL-17A, or both IL-17A and IL-17F polypeptide molecules. IL-17A and IL-17F are cytokines that are involved in inflammatory processes and human disease. IL-17RC is a common receptor for IL-17A and IL-17F. The present invention includes methods of using a soluble IL-17RC receptor, IL-17RCx4 for treating inflammation.
摘要翻译: 本发明涉及阻断,抑制,降低,拮抗或中和IL-17F,IL-17A或IL-17A和IL-17F两者多肽分子的活性。 IL-17A和IL-17F是参与炎症过程和人类疾病的细胞因子。 IL-17RC是IL-17A和IL-17F的常见受体。 本发明包括使用可溶性IL-17RC受体IL-17RCx4来治疗炎症的方法。
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公开(公告)号:US20100113748A1
公开(公告)日:2010-05-06
申请号:US12580112
申请日:2009-10-15
申请人: Rolf E. Kuestner , Zeren Gao , Steven D. Levin , Mark W. Rixon
发明人: Rolf E. Kuestner , Zeren Gao , Steven D. Levin , Mark W. Rixon
CPC分类号: C07K14/7155 , A61K38/00 , A61K2121/00 , C07K14/715 , C07K16/2866 , C07K2317/73 , C07K2317/76 , C07K2319/21 , C07K2319/30 , C07K2319/43
摘要: The present invention relates to blocking, inhibiting, reducing, antagonizing or neutralizing the activity of IL-17F, IL-17A, or both IL-17A and IL-17F polypeptide molecules. IL-17A and IL-17F are cytokines that are involved in inflammatory processes and human disease. IL-17RC is a common receptor for IL-17A and IL-17F. The present invention includes methods of using a soluble IL-17RC receptor, IL-17RCx4 for treating inflammation.
摘要翻译: 本发明涉及阻断,抑制,降低,拮抗或中和IL-17F,IL-17A或IL-17A和IL-17F两者多肽分子的活性。 IL-17A和IL-17F是参与炎症过程和人类疾病的细胞因子。 IL-17RC是IL-17A和IL-17F的常见受体。 本发明包括使用可溶性IL-17RC受体IL-17RCx4来治疗炎症的方法。
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公开(公告)号:US07122632B2
公开(公告)日:2006-10-17
申请号:US09745792
申请日:2000-12-22
申请人: Donald C. Foster , Wenfeng Xu , Karen L. Madden , James D. Kelly , Cindy A. Sprecher , Cameron S. Brandt , Mark W. Rixon , Scott R. Presnell , Brian A. Fox
发明人: Donald C. Foster , Wenfeng Xu , Karen L. Madden , James D. Kelly , Cindy A. Sprecher , Cameron S. Brandt , Mark W. Rixon , Scott R. Presnell , Brian A. Fox
IPC分类号: C07K14/705 , C12P21/02
CPC分类号: C07K16/2866 , A61K38/00 , C07K14/7155 , C07K2319/00
摘要: A soluble receptor to IL-20 having two polypeptide subunits, IL-20RA (formerly called ZcytoR7) and IL-20RB (formerly called DIRS1). The two subunits are preferably linked together. In one embodiment one subunit is fused to the constant region of the light chain of an immunoglobulin, and the other subunit is fused to the constant region of the heavy chain of the immunoglobulin. The light chain and the heavy chain are connected via a disulfide bond.
摘要翻译: 具有两个多肽亚单位IL-20RA(以前称为ZcytoR7)和IL-20RB(以前称为DIRS1)的IL-20的可溶性受体。 两个亚基优选连接在一起。 在一个实施方案中,一个亚基与免疫球蛋白的轻链的恒定区融合,另一个亚基与免疫球蛋白的重链的恒定区融合。 轻链和重链通过二硫键连接。
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公开(公告)号:US06207815B1
公开(公告)日:2001-03-27
申请号:US08479285
申请日:1995-06-07
申请人: Peter S. Mezes , Brian B. Gourlie , Mark W. Rixon , Jeffrey Schlom , Donald A. Kaplan , W. H. Kerr Anderson
发明人: Peter S. Mezes , Brian B. Gourlie , Mark W. Rixon , Jeffrey Schlom , Donald A. Kaplan , W. H. Kerr Anderson
IPC分类号: C12N1514
CPC分类号: C07K16/462 , A61K38/00 , A61K47/6877 , A61K51/1087 , A61K2123/00 , C07K16/30 , C07K2317/24 , C07K2319/00
摘要: This invention concerns a family of chimeric antibodies with high affinities to a high molecular weight, tumor-associated sialylated glycoprotein antigen (TAG-72) of human origin. These antibodies have (1) high affinity animal VH and VL sequences which mediate TAG-72 binding and (2) human CH and CL regions. They are thought to produce significantly fewer side-effects when administered to human patients by virtue of their human CH and CL antibody domains. The nucleotide and amino acid sequences of VH&agr;TAG VH, CC46 VH, CC49H, CC83 VH, and CC92 VH, and CC49L, CC83 VL, and CC92 VL idiotype sequences are disclosed, as well as in vivo methods of treatment and diagnostic assay using these chimeric antibodies.
摘要翻译: 本发明涉及对人类高分子量肿瘤相关唾液酸化糖蛋白抗原(TAG-72)具有高亲和力的嵌合抗体家族。 这些抗体具有(1)介导TAG-72结合的高亲和力动物VH和VL序列,(2)人CH和CL区。 据认为,由于其人类CH和CL抗体结构域,当向人类患者施用时,它们会产生显着较少的副作用。 公开了VHαphaVV,CC46VH,CC49H,CC83VV和CC92VV,CC49L,CC83VL和CC92VV独立型序列的核苷酸和氨基酸序列,以及使用这些嵌合体的体内治疗和诊断测定方法 抗体。
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公开(公告)号:US5993813A
公开(公告)日:1999-11-30
申请号:US822028
申请日:1997-03-24
申请人: Peter S. Mezes , Brian B. Gourlie , Mark W. Rixon , Jeffrey Schlom , Donald A. Kaplan , W. H. Kerr Anderson
发明人: Peter S. Mezes , Brian B. Gourlie , Mark W. Rixon , Jeffrey Schlom , Donald A. Kaplan , W. H. Kerr Anderson
IPC分类号: A61K38/00 , A61K47/48 , A61K51/10 , A61P35/00 , C07K16/30 , C07K16/46 , C12N15/14 , C12P21/08 , A61K39/395
CPC分类号: A61K47/48669 , A61K51/1087 , C07K16/30 , C07K16/462 , A61K2123/00 , A61K38/00 , C07K2317/24 , C07K2319/00
摘要: This invention concerns a family of chimeric antibodies with high affinities to a high molecular weight, tumor-associated sialylated glycoprotein antigen (TAG-72) of human origin. These antibodies have (1) high affinity animal V.sub.H and V.sub.L sequences which mediate TAG-72 binding and (2) human C.sub.H and C.sub.L regions. They are thought to produce significantly fewer side-effects when administered to human patients by virtue of their human C.sub.H and C.sub.L antibody domains. The nucleotide and amino acid sequences of V.sub.H .alpha.TAG V.sub.H, CC46 V.sub.H, CC49.sub.H, CC83 V.sub.H, and CC92 V.sub.H, and CC49.sub.L, CC83 V.sub.L, and CC92 V.sub.L idiotype sequences are disclosed, as well as in vivo methods of treatment and diagnostic assay using these chimeric antibodies.
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公开(公告)号:US5808033A
公开(公告)日:1998-09-15
申请号:US471426
申请日:1995-06-06
申请人: Brian B. Gourlie , Mark W. Rixon , Peter S. Mezes
发明人: Brian B. Gourlie , Mark W. Rixon , Peter S. Mezes
IPC分类号: C12N15/09 , A61K38/00 , A61K39/395 , A61P35/00 , C07K16/30 , C07K16/32 , C12N15/13 , C12P21/08 , C12R1/91 , C07H21/04
CPC分类号: C07K16/3007 , A61K38/00 , C07K2317/24
摘要: The present invention discloses novel chimeric monoclonal antibodies directed against human carcinoembryonic antigen, having antigen-specific variable regions. DNA constructs for the light and heavy chain variable regions comprising the novel antibodies of the invention are also disclosed. Eukaryotic host cells capable of expression of the chimeric antibodies and comprising the novel chimeric antibody-encoding DNA constructs are also described.
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公开(公告)号:US5472693A
公开(公告)日:1995-12-05
申请号:US17570
申请日:1993-02-16
IPC分类号: C12N15/09 , A61K38/00 , A61K39/395 , A61P35/00 , C07K16/30 , C07K16/32 , C12N15/13 , C12P21/08 , C12R1/91 , C07K16/28
CPC分类号: C07K16/3007 , A61K38/00 , C07K2317/24
摘要: The present invention discloses novel chimeric monoclonal antibodies directed against human carcinoembryonic antigen, having antigen-specific variable regions. DNA constructs for the light and heavy chain variable regions comprising the novel antibodies of the invention are also disclosed. Eukaryotic host cells capable of expression of the chimeric antibodies and comprising the novel chimeric antibody-encoding DNA constructs are also described.
摘要翻译: 本发明公开了针对人癌胚抗原的新型嵌合单克隆抗体,其具有抗原特异性可变区。 还公开了包含本发明新抗体的轻链和重链可变区的DNA构建体。 还描述了能够表达嵌合抗体并且包含新的嵌合抗体编码DNA构建体的真核宿主细胞。
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38.发明申请METHODS OF TREATING INFLAMMATION USING SOLUBLE IL-17RA/RC FUSION PROTEINS 审中-公开使用可溶性IL-17RA / RC融合蛋白治疗炎症的方法公开(公告)号:US20120289684A1
公开(公告)日:2012-11-15
申请号:US13487828
申请日:2012-06-04
申请人: Steven D. Levin , Mark W. Rixon , Zeren Gao
发明人: Steven D. Levin , Mark W. Rixon , Zeren Gao
CPC分类号: C07K14/7155 , A61K2039/505 , C07K16/2866 , C07K2317/73 , C07K2317/76 , C07K2319/30 , C07K2319/32
摘要: Disclosed are antagonists of IL-17A and IL-17F. The antagonists are based on soluble IL-17RA and IL-17RC fusion proteins, including hybrid soluble receptors comprising portions of both IL-17RC and IL-17RA (“IL-17RC/IL-17RA”). Such antagonists serve to block, inhibit, reduce, antagonize or neutralize the activity of IL-17F, IL-17A, or both IL-17A and IL-17F. Also disclosed are methods of using such antagonists for treating disease, particularly inflammatory diseases mediated at least in part by IL-17A and/or IL-17F.
摘要翻译: 公开了IL-17A和IL-17F的拮抗剂。 拮抗剂基于可溶性IL-17RA和IL-17RC融合蛋白,包括包含IL-17RC和IL-17RA(IL-17RC / IL-17RA)部分的杂合可溶性受体。 这种拮抗剂用于阻断,抑制,降低,拮抗或中和IL-17F,IL-17A或IL-17A和IL-17F两者的活性。 还公开了使用这种拮抗剂治疗疾病,特别是至少部分地由IL-17A和/或IL-17F介导的炎性疾病的方法。
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公开(公告)号:US20110217291A1
公开(公告)日:2011-09-08
申请号:US12999564
申请日:2009-06-29
申请人: Carl W. Birks , Brian A. Fox , Mark W. Rixon , Jeff L. Ellsworth
发明人: Carl W. Birks , Brian A. Fox , Mark W. Rixon , Jeff L. Ellsworth
IPC分类号: A61K39/395 , C12N15/63 , C12P21/02 , C12N5/10 , C07K16/42 , C12N1/00 , C07H21/00 , A61P29/00 , A61P19/02
CPC分类号: C07K14/70503 , A61K38/00 , C07K14/70535
摘要: Disclosed are soluble hybrid Fcγ receptor (FcγR) polypeptide compositions and related methods of using such polypeptides to treat IgG-mediated and immune complex-mediated inflammation. Also disclosed are related compositions and methods for producing the soluble hybrid FcγR polypeptides.
摘要翻译: 公开了可溶性杂合Fcγ受体(FcγR)多肽组合物和使用这些多肽治疗IgG介导的和免疫复合物介导的炎症的相关方法。 还公开了用于产生可溶性杂合FcγR多肽的相关组合物和方法。
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公开(公告)号:US20100197575A1
公开(公告)日:2010-08-05
申请号:US12509667
申请日:2009-07-27
申请人: Donald C. Foster , Wenfeng Xu , Karen L. Madden , James D. Kelly , Cindy A. Sprecher , Cameron S. Brandt , Mark W. Rixon , Scott R. Presnell , Brian A. Fox
发明人: Donald C. Foster , Wenfeng Xu , Karen L. Madden , James D. Kelly , Cindy A. Sprecher , Cameron S. Brandt , Mark W. Rixon , Scott R. Presnell , Brian A. Fox
CPC分类号: C07K16/2866 , A61K38/00 , C07K14/7155 , C07K2319/00
摘要: A soluble receptor to IL-20 having two polypeptide subunits, IL-20RA (formerly called ZcytoR7) and IL-20RB (formerly called DIRS1). The two subunits are preferably linked together. In one embodiment one subunit is fused to the constant region of the light chain of an immunoglobulin, and the other subunit is fused to the constant region of the heavy chain of the immunoglobulin. The light chain and the heavy chain are connected via a disulfide bond.
摘要翻译: 具有两个多肽亚单位IL-20RA(以前称为ZcytoR7)和IL-20RB(以前称为DIRS1)的IL-20的可溶性受体。 两个亚基优选连接在一起。 在一个实施方案中,一个亚基与免疫球蛋白的轻链的恒定区融合,另一个亚基与免疫球蛋白的重链的恒定区融合。 轻链和重链通过二硫键连接。
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