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    • 5. 发明申请
    • HUMANIZED FcγRIIB SPECIFIC ANTIBODIES AND METHODS OF USE THEREOF
    • 人类FcγRIIB特异性抗体及其使用方法
    • WO2005110474A2
    • 2005-11-24
    • PCT/US2005/016260
    • 2005-05-10
    • MACROGENICS, INC.JOHNSON, Leslie, S.HUANG, Ling
    • JOHNSON, Leslie, S.HUANG, Ling
    • A61K39/395
    • C07K16/283A61K2039/505C07K2317/24C07K2317/34
    • The present invention relates to humanized FcγRIIB antibodies, fragments, and variants thereof that bind human FcγRIIB with a greater affinity than said antibody binds FcγRIIA. The invention encompasses the use of the humanized antibodies of the invention for the treatment of any disease related to loss of balance of Fc receptor mediated signaling, such as cancer, autoimmune and inflammatory disease. The invention provides methods of enhancing the therapeutic effect of therapeutic antibodies by administering the humanized antibodies of the invention to enhance the effector function of the therapeutic antibodies. The invention also provides methods of enhancing the efficacy of a vaccine composition by administering the humanized antibodies of the invention. The invention encompasses methods for treating an autoimmune disease and methods for elimination of cancer cells that express FcγRIIB.
    • 本发明涉及以与抗体结合FcγRIIA更大的亲和力结合人FcγRIIB的人源化FcγRIIB抗体,其片段和变体。 本发明包括本发明的人源化抗体用于治疗与Fc受体介导的信号传导的平衡失去相关的任何疾病(例如癌症,自身免疫性和炎性疾病)的用途。 本发明提供了通过施用本发明的人源化抗体来增强治疗性抗体的治疗效果以增强治疗性抗体的效应子功能的方法。 本发明还提供了通过施用本发明的人源化抗体来增强疫苗组合物的功效的方法。 本发明包括治疗自身免疫疾病的方法和用于消除表达FcγRIIB的癌细胞的方法。
    • 7. 发明申请
    • NOVEL B7-H3 BINDING MOLECULES, ANTIBODY DRUG CONJUGATES THEREOF AND METHODS OF USE THEREOF
    • 新的B7-H3结合分子,抗体药物偶联物及其使用方法
    • WO2017180813A1
    • 2017-10-19
    • PCT/US2017/027317
    • 2017-04-13
    • MACROGENICS, INC.
    • LOO, Deryk, T.HUANG, LingJOHNSON, Leslie, S.SON, ThomasSCRIBNER, JuniperBONVINI, Ezio
    • A61K39/395A61K47/68C07K16/28
    • The present invention is directed to novel B7-H3-binding molecules capable of binding to human and non-human B7-H3, and in particular to such molecules that are cross-reactive with B7-H3 of a non-human primate (e.g., a cynomolgus monkey). The invention additionally pertains to B7-H3-binding molecules that comprise Variable Light Chain and/or Variable Heavy Chain (VH) Domains that have been humanized and/or deimmunized so as to exhibit a reduced immunogenicity upon administration to recipient subjects. The invention particularly pertains to bispecific, trispecific or multispecific B7-H3-binding molecules, including bispecific diabodies, BiTEs, bispecific antibodies, trivalent binding molecules, etc. that comprise: (i) such B7-H3-binding Variable Domains and (ii) a domain capable of binding to an epitope of a molecule present on the surface of an effector cell. The invention also particularly pertains to a molecule that comprises the human B7-H3 binding domain of a humanized anti-human B7-H3 antibody conjugated to at least one drug moiety (a "B7-H3-ADC").
    • 本发明涉及能够结合人和非人B7-H3的新型B7-H3结合分子,特别是涉及与B7-H3交叉反应的分子 非人灵长类动物(例如食蟹猴)。 本发明另外涉及包含可变轻链和/或可变重链(VH)结构域的B7-H3结合分子,所述可变轻链和/或可变重链(VH)结构域已被人源化和/或去免疫化,以便在给予受体对象时表现出降低的免疫原性。 本发明特别涉及双特异性,三特异性或多特异性B7-H3结合分子,包括双特异性双抗体,BiTE,双特异性抗体,三价结合分子等,其包含:(i)此类结合B7-H3的可变结构域和(ii) 能够结合存在于效应细胞表面上的分子的表位的结构域。 本发明还特别涉及包含与至少一个药物部分(“B7-H3-ADC”)缀合的人源化抗人B7-H3抗体的人B7-H3结合结构域的分子。