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公开(公告)号:US20120020965A1
公开(公告)日:2012-01-26
申请号:US13034144
申请日:2011-02-24
IPC分类号: A61K39/395 , C12N15/62 , C12N15/63 , A61P31/00 , C12N1/21 , C12P21/00 , A61P37/04 , A61P35/00 , C07K19/00 , C12N5/10
CPC分类号: C07K16/2896 , A61K39/39541 , A61K39/39558 , A61K2039/505 , C07K16/28 , C07K16/30 , C07K2317/14 , C07K2317/24 , C07K2317/52 , C07K2317/54 , C07K2317/622 , C07K2317/64 , C07K2317/71 , C07K2317/73 , C07K2317/74 , C12N5/0635 , C12N2501/056 , C12N2501/599
摘要: The present invention provides novel CD180 binding molecules, methods for their identification, and methods for their use.
摘要翻译: 本发明提供新颖的CD180结合分子,其鉴定方法及其使用方法。
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公开(公告)号:US09260529B2
公开(公告)日:2016-02-16
申请号:US13034144
申请日:2011-02-24
IPC分类号: C07K16/28 , C12N5/0781 , C07K16/30 , A61K39/395
CPC分类号: C07K16/2896 , A61K39/39541 , A61K39/39558 , A61K2039/505 , C07K16/28 , C07K16/30 , C07K2317/14 , C07K2317/24 , C07K2317/52 , C07K2317/54 , C07K2317/622 , C07K2317/64 , C07K2317/71 , C07K2317/73 , C07K2317/74 , C12N5/0635 , C12N2501/056 , C12N2501/599
摘要: The present invention provides novel CD180 binding molecules, methods for their identification, and methods for their use.
摘要翻译: 本发明提供新颖的CD180结合分子,其鉴定方法及其使用方法。
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公开(公告)号:US20070237779A1
公开(公告)日:2007-10-11
申请号:US10566409
申请日:2003-12-24
IPC分类号: A61K39/395 , C07K16/30
CPC分类号: C07K16/2809 , A61K2039/505 , C07K16/2818 , C07K16/2878 , C07K16/2896 , C07K16/462 , C07K16/464 , C07K2317/22 , C07K2317/24 , C07K2317/31 , C07K2317/52 , C07K2317/522 , C07K2317/524 , C07K2317/526 , C07K2317/53 , C07K2317/56 , C07K2317/565 , C07K2317/622 , C07K2317/72 , C07K2317/73 , C07K2317/732 , C07K2317/734 , C07K2317/94 , C07K2319/00 , C07K2319/30 , C07K2319/32
摘要: The invention relates to novel binding domain-immunoglobulin fusion proteins that feature a binding domain for a cognate structure such as an antigen, a counterreceptor or the like, a wild-type IgG, IGA or IgE hinge-acting region, i.e., IgE CH2, region polypeptide or a mutant IgGI hinge region polypeptide having either zero, one or two cysteine residues, and immunoglobulin CH2 and CH3 domains, and that are capable of ADCC and/or CDC while occurring predominantly as polypeptides that are compromised in their ability to form disulfide-linked multimers. The fusion proteins can be recombinantly produced at high expression levels. Also provided are related compositions and methods, including cell surface forms of the fusion proteins and immunotherapeutic applications of the fusion proteins and of polynucleotides encoding such fusion proteins.
摘要翻译: 本发明涉及新颖的结合域 - 免疫球蛋白融合蛋白,其特征在于一种同源结构的结合域,例如抗原,反向受体等,野生型IgG,IGA或IgE铰链作用区,即IgE CH2, 区域多肽或具有零个,一个或两个半胱氨酸残基和免疫球蛋白CH2和CH3结构域的突变IgG1铰链区多肽,并且能够产生ADCC和/或CDC,同时主要作为其形成二硫键的能力受损的多肽 链接的多聚体。 可以以高表达水平重组产生融合蛋白。 还提供了相关的组合物和方法,包括融合蛋白的细胞表面形式和融合蛋白的免疫治疗应用以及编码这种融合蛋白的多核苷酸。
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公开(公告)号:US20050175614A1
公开(公告)日:2005-08-11
申请号:US11089511
申请日:2005-03-23
IPC分类号: C07K16/28 , C07K16/46 , A61K39/395
CPC分类号: C07K16/46 , A61K2039/505 , C07K16/2809 , C07K16/2818 , C07K16/2878 , C07K16/2896 , C07K16/462 , C07K2317/22 , C07K2317/24 , C07K2317/53 , C07K2317/622 , C07K2317/64 , C07K2317/732 , C07K2317/734 , C07K2319/00 , C07K2319/30
摘要: The invention relates to novel binding domain-immunoglobulin fusion proteins that feature a binding domain for a cognate structure such as an antigen, a counterreceptor or the like, a hinge region polypeptide having either zero or one cysteine residue, and immunoglobulin CH2 and CH3 domains, and that are capable of ADCC and/or CDC while occurring predominantly as monomeric polypeptides. The fusion proteins can be recombinantly produced at high expression levels. Also provided are related compositions and methods, including immunotherapeutic applications.
摘要翻译: 本发明涉及新颖的结合域 - 免疫球蛋白融合蛋白,其特征在于用于相关结构的结合域,例如抗原,反式受体等,具有零个或一个半胱氨酸残基的铰链区多肽,以及免疫球蛋白CH 2和CH 3 结构域,并且其能够主要以单体多肽的形式存在于ADCC和/或CDC。 可以以高表达水平重组产生融合蛋白。 还提供了相关的组合物和方法,包括免疫治疗应用。
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公开(公告)号:US20050202023A1
公开(公告)日:2005-09-15
申请号:US11088569
申请日:2005-03-23
IPC分类号: C07K16/28 , C07K16/46 , A61K39/395
CPC分类号: C07K16/46 , A61K2039/505 , C07K16/2809 , C07K16/2818 , C07K16/2878 , C07K16/2896 , C07K16/462 , C07K2317/22 , C07K2317/24 , C07K2317/53 , C07K2317/622 , C07K2317/64 , C07K2317/732 , C07K2317/734 , C07K2319/00 , C07K2319/30
摘要: The invention relates to novel binding domain-immunoglobulin fusion proteins that feature a binding domain for a cognate structure such as an antigen, a counterreceptor or the like, a hinge region polypeptide having either zero or one cysteine residue, and immunoglobulin CH2 and CH3 domains, and that are capable of ADCC and/or CDC while occurring predominantly as monomeric polypeptides. The fusion proteins can be recombinantly produced at high expression levels. Also provided are related compositions and methods, including immunotherapeutic applications.
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公开(公告)号:US20050136049A1
公开(公告)日:2005-06-23
申请号:US10627556
申请日:2003-07-26
IPC分类号: C07K16/28 , C07K16/46 , A61K39/395 , C07K16/44
CPC分类号: C07K16/2809 , A61K2039/505 , C07K16/2818 , C07K16/2878 , C07K16/2896 , C07K16/462 , C07K16/464 , C07K2317/22 , C07K2317/24 , C07K2317/53 , C07K2317/56 , C07K2317/622 , C07K2317/64 , C07K2317/732 , C07K2317/734 , C07K2319/00 , C07K2319/30
摘要: The invention relates to novel binding domain-immunoglobulin fusion proteins that feature a binding domain for a cognate structure such as an antigen, a counterreceptor or the like, a wild-type IgG1, IGA or IgE hinge-acting region, i.e., IgE CH2, region polypeptide or a mutant IgG1 hinge region polypeptide having either zero, one or two cysteine residues, and immunoglobulin CH2 and CH3 domains, and that are capable of ADCC and/or CDC while occurring predominantly as polypeptides that are compromised in their ability to form disulfide-linked multimers. The fusion proteins can be recombinantly produced at high expression levels. Also provided are related compositions and methods, including cell surface forms of the fusion proteins and immunotherapeutic applications of the fusion proteins and of polynucleotides encoding such fusion proteins.
摘要翻译: 本发明涉及新颖的结合域 - 免疫球蛋白融合蛋白,其特征在于一种同源结构的结合域,例如抗原,反向受体等,野生型IgG1,IGA或IgE铰链作用区,即IgE CH2, 区域多肽或具有零个,一个或两个半胱氨酸残基和免疫球蛋白CH2和CH3结构域的突变IgG1铰链区多肽,并且能够产生ADCC和/或CDC,同时主要作为其形成二硫键的能力受损的多肽 链接的多聚体。 可以以高表达水平重组产生融合蛋白。 还提供了相关的组合物和方法,包括融合蛋白的细胞表面形式和融合蛋白的免疫治疗应用以及编码这种融合蛋白的多核苷酸。
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7.发明申请公开(公告)号:US20070025982A1
公开(公告)日:2007-02-01
申请号:US11542423
申请日:2006-10-03
IPC分类号: A61K39/395 , A61K39/12
CPC分类号: C07K14/005 , A61K39/00 , A61K39/12 , A61K39/21 , A61K2039/53 , A61K2039/57 , A61K2039/6031 , C07K2319/00 , C12N2740/16122 , C12N2740/16134
摘要: Vaccines that target one or more antigens to a cell surface receptor improve the antigen-specific humoral and cellular immune response. Antigen(s) linked to a domain that binds to a cell surface receptor are internalized, carrying antigen(s) into an intracellular compartment where the antigen(s) are digested into peptides and loaded onto MHC molecules. T cells specific for the peptide antigens are activated, leading to an enhanced immune response. The vaccine may comprise antigen(s) linked to a domain that binds at least one receptor or a DNA plasmid encoding antigen(s) linked to a domain that binds at least one receptor. A preferred embodiment of the invention targets HIV-1 env antigen to the CD40 receptor, resulting in delivery of antigen to CD40 positive cells, and selective activation of the CD40 receptor on cells presenting HIV-1 env antigens to T cells.
摘要翻译: 将一种或多种抗原靶向细胞表面受体的疫苗可改善抗原特异性体液和细胞免疫应答。 与结合细胞表面受体的结构域连接的抗原被内化,将抗原携带到细胞内隔室中,其中抗原被消化成肽并加载到MHC分子上。 对肽抗原特异性的T细胞被激活,导致增强的免疫应答。 疫苗可以包含连接到结合至少一种受体的结构域的抗原或编码与结合至少一种受体的结构域连接的抗原的DNA质粒。 本发明的优选实施方案将HIV-1 env抗原靶向CD40受体,导致抗原递送至CD40阳性细胞,以及将呈递HIV-1 env抗原的细胞上的CD40受体选择性激活至T细胞。
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公开(公告)号:US20050202028A1
公开(公告)日:2005-09-15
申请号:US11088693
申请日:2005-03-23
IPC分类号: C07K16/28 , C07K16/46 , A61K39/395
CPC分类号: C07K16/46 , A61K2039/505 , C07K16/2809 , C07K16/2818 , C07K16/2878 , C07K16/2896 , C07K16/462 , C07K2317/22 , C07K2317/24 , C07K2317/53 , C07K2317/622 , C07K2317/64 , C07K2317/732 , C07K2317/734 , C07K2319/00 , C07K2319/30
摘要: The invention relates to novel binding domain-immunoglobulin fusion proteins that feature a binding domain for a cognate structure such as an antigen, a counterreceptor or the like, a hinge region polypeptide having either zero or one cysteine residue, and immunoglobulin CH2 and CH3 domains, and that are capable of ADCC and/or CDC while occurring predominantly as monomeric polypeptides. The fusion proteins can be recombinantly produced at high expression levels. Also provided are related compositions and methods, including immunotherapeutic applications.
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公开(公告)号:US20050186216A1
公开(公告)日:2005-08-25
申请号:US11088570
申请日:2005-03-23
IPC分类号: C07K16/28 , C07K16/46 , A61K39/395
CPC分类号: C07K16/46 , A61K2039/505 , C07K16/2809 , C07K16/2818 , C07K16/2878 , C07K16/2896 , C07K16/462 , C07K2317/22 , C07K2317/24 , C07K2317/53 , C07K2317/622 , C07K2317/64 , C07K2317/732 , C07K2317/734 , C07K2319/00 , C07K2319/30
摘要: The invention relates to novel binding domain-immunoglobulin fusion proteins that feature a binding domain for a cognate structure such as an antigen, a counterreceptor or the like, a hinge region polypeptide having either zero or one cysteine residue, and immunoglobulin CH2 and CH3 domains, and that are capable of ADCC and/or CDC while occurring predominantly as monomeric polypeptides. The fusion proteins can be recombinantly produced at high expression levels. Also provided are related compositions and methods, including immunotherapeutic applications.
摘要翻译: 本发明涉及新颖的结合域 - 免疫球蛋白融合蛋白,其特征在于同源结构如结合抗原,反式受体等的结合结构域,具有零个或一个半胱氨酸残基的铰链区多肽和免疫球蛋白CH2和CH3结构域, 并且其能够主要以单体多肽的形式存在于ADCC和/或CDC。 可以以高表达水平重组产生融合蛋白。 还提供了相关的组合物和方法,包括免疫治疗应用。
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10.发明申请B-cell reduction using CD37-specific and CD20-specific binding molecules 审中-公开使用CD37特异性和CD20特异性结合分子的B细胞减少公开(公告)号:US20070059306A1
公开(公告)日:2007-03-15
申请号:US11493132
申请日:2006-07-25
申请人: Laura Grosmaire , Martha Hayden-Ledbetter , Jeffrey Ledbetter , Peter Thompson , Sandy Simon , William Brady
发明人: Laura Grosmaire , Martha Hayden-Ledbetter , Jeffrey Ledbetter , Peter Thompson , Sandy Simon , William Brady
IPC分类号: A61K39/395
CPC分类号: A61K39/3955 , A61K39/39558 , A61K45/06 , A61K2039/505 , A61K2039/507 , A61K2039/545 , C07K16/2887 , C07K16/2896 , C07K16/30 , C07K16/3061 , C07K2317/24 , C07K2317/52 , C07K2317/53 , C07K2317/56 , C07K2317/565 , C07K2317/567 , C07K2317/622 , C07K2317/72 , C07K2317/73 , C07K2317/732 , C07K2317/734 , C07K2317/75 , C07K2317/76 , A61K2300/00
摘要: The present invention generally provides methods for B-cell reduction in an individual using CD37-specific binding molecules. In particular, the invention provides methods for B-cell reduction using CD37-specific binding molecules alone, or a combination of CD37-specific binding molecules and CD20-specific binding molecules, in some instances a synergistic combination. The invention further provides materials and methods for treatment of diseases involving aberrant B-cell activity. In addition, the invention provides humanized CD37-specific binding molecules.
摘要翻译: 本发明通常提供使用CD37特异性结合分子的个体中B细胞减少的方法。 特别地,本发明提供了使用单独的CD37-特异性结合分子或CD37-特异性结合分子和CD20-特异性结合分子的组合(在某些情况下是协同组合)的B细胞减少的方法。 本发明还提供了用于治疗涉及异常B细胞活性的疾病的材料和方法。 此外,本发明提供了人源化的CD37特异性结合分子。
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