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1.发明授权Soluble interleukin-2 receptor as a disease indicator and a method of assaying the same 失效可溶性白介素-2受体作为疾病指标及其分析方法
公开(公告)号:US4707443A
公开(公告)日:1987-11-17
申请号:US724897
申请日:1985-04-19
申请人: David Nelson , William Biddison , Laurence Rubin , Warner Greene , Warren Leonard , Robert Yarchoan
发明人: David Nelson , William Biddison , Laurence Rubin , Warner Greene , Warren Leonard , Robert Yarchoan
IPC分类号: G01N33/53 , A61K35/14 , A61K38/00 , C07K14/005 , C07K14/195 , C07K14/705 , C07K16/00 , C07K16/28 , C07K19/00 , C12N5/10 , C12N15/02 , C12P21/00 , C12P21/08 , C12R1/91 , G01N33/577 , G01N33/68 , C12N15/00
CPC分类号: G01N33/6869 , C07K16/2866 , Y10S435/81 , Y10S435/966 , Y10S435/967 , Y10S435/969 , Y10S435/975 , Y10S436/80 , Y10S436/808 , Y10S436/809 , Y10S436/813 , Y10S530/868
摘要: The present invention discloses a sandwich method and a kit for assaying interleukin-2 receptor (IL-2R) in a sample. The method comprises determining reactivity of said sample with a plurality of ligands, each said ligand having binding affinity for a specific site on the receptor, said site being different for each said ligand and distinct from interleukin-2 binding site on the receptor. The invention also discloses a method of detecting such disturbed or abnormal conditions in humans which release soluble IL-2R in the body fluid.
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公开(公告)号:US20050249712A1
公开(公告)日:2005-11-10
申请号:US11084408
申请日:2005-03-18
申请人: Warren Leonard , Akhilesh Pandey , Amin Al-Shami , Rosanne Spolski , John Kelly , Andrea Keane-Myers
发明人: Warren Leonard , Akhilesh Pandey , Amin Al-Shami , Rosanne Spolski , John Kelly , Andrea Keane-Myers
IPC分类号: A61K31/7088 , A61K35/17 , A61K35/18 , A61K38/18 , A61K38/19 , A61K38/20 , A61K39/00 , A61K41/00 , A61K45/00
CPC分类号: A61K35/17 , A01K67/0276 , A01K2217/075 , A01K2217/15 , A01K2227/105 , A01K2267/0387 , A61K9/0078 , A61K31/7088 , A61K38/00 , A61K41/00 , A61K45/06 , A61K48/00 , A61K2039/505 , C07K14/5418 , C07K16/244 , A61K2300/00
摘要: Methods are disclosed herein for specifically inducing proliferation of CD4+ T cells. The methods are of use in treating immunodeficiencies, such as an immunodeficiency produced by infection with an immunodeficiency virus, such as infection with a human immunodeficiency virus (HIV). The methods include contacting isolated mammalian CD4+ T cells with an effective amount of a thymic stromal derived lymphopoietin (TSLP) polypeptide or a therapeutically effective amount of nucleic acid encoding the TSLP polypeptide, thereby inducing proliferation of the T cells. Methods are also disclosed for treating an IgE mediated disorder, such as asthma. The methods include administering to a subject a therapeutically effective amount of a TSLP antagonist. Transgenic mice are also disclosed herein. The somatic and germ cells of these mice include a disrupted thymic stromal lymphopoietin receptor (TSLP) gene, the disruption being sufficient to inhibit the interaction of TSLP with its receptor, and a disrupted γc gene, the disruption being sufficient to reduce signaling through the γc. The mice exhibit diminished thymic cellularity. Methods of using these mice for drug screening are also disclosed.
摘要翻译: 本文公开了用于特异性诱导CD4 + T细胞增殖的方法。 该方法可用于治疗免疫缺陷,例如由免疫缺陷病毒感染产生的免疫缺陷,例如人免疫缺陷病毒(HIV)的感染。 所述方法包括使分离的哺乳动物CD4 + T细胞与有效量的胸腺基质衍生的淋巴细胞生成素(TSLP)多肽或治疗有效量的编码TSLP多肽的核酸接触,从而诱导T细胞的增殖。 还公开了用于治疗IgE介导的病症如哮喘的方法。 所述方法包括向受试者施用治疗有效量的TSLP拮抗剂。 本文还公开了转基因小鼠。 这些小鼠的体细胞和生殖细胞包括破坏的胸腺基质淋巴细胞生成素受体(TSLP)基因,破坏足以抑制TSLP与其受体的相互作用,以及破坏的γ基因,破坏 足以减少信号通过伽马。 小鼠表现出胸腺细胞减少。 还公开了将这些小鼠用于药物筛选的方法。
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公开(公告)号:US20050170410A1
公开(公告)日:2005-08-04
申请号:US11052527
申请日:2005-02-07
申请人: Akhilesh Pandey , Katsutoshi Ozaki , Heinz Baumann , Steven Levin , Andrew Farr , Warren Leonard , Harvey Lodish
发明人: Akhilesh Pandey , Katsutoshi Ozaki , Heinz Baumann , Steven Levin , Andrew Farr , Warren Leonard , Harvey Lodish
CPC分类号: C07K14/7155 , A61K38/00 , C07K2319/30
摘要: The present invention provides Thymic Stromal Lymphopoietin Receptor (TSLPR) polypeptides and nucleic acid molecules encoding the same. The invention also provides selective binding agents, vectors, host cells, and methods for producing TSLPR polypeptides. The invention further provides pharmaceutical compositions and methods for the diagnosis, treatment, amelioration, and/or prevention of diseases, disorders, and conditions associated with TSLPR polypeptides.
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公开(公告)号:US20100135958A1
公开(公告)日:2010-06-03
申请号:US12651858
申请日:2010-01-04
申请人: Patrick Hwu , Gang Wang , Warren Leonard , Rosanne Spolski , Katsutoshi Ozaki
发明人: Patrick Hwu , Gang Wang , Warren Leonard , Rosanne Spolski , Katsutoshi Ozaki
IPC分类号: A61K38/20 , A61K31/7088 , A61P37/00
CPC分类号: A61K38/2013 , A61K38/20 , A61K38/2046 , A61K38/2086 , A61K39/0011 , A61K48/005 , A61K2039/55527 , A61K2300/00
摘要: A method of treating and/or preventing cancer in a subject, preferably mammalian, more preferably human, by administering in an effective amount IL-21 polypeptide, polynucleotide, vector comprising an IL-21 nucleic acid sequence encoding an IL-21 polypeptide, variants, and fragments thereof, thereby acting as an anti-cancer agent by reducing, ameliorating, and/or eliminating the cancer; and a method of treating and/or preventing cancer in a subject by co-administering the IL-21 polypeptide, polynucleotide, IL-21 vector, variant, and fragments thereof, with an immunotherapeutic and/or chemotherapeutic agent for the treatment and/or prevention of cancer in a subject.
摘要翻译: 通过施用有效量的IL-21多肽,多核苷酸,包含编码IL-21多肽的IL-21核酸序列的载体的载体,变体(或其组合)的变体,治疗和/或预防受试者,优选哺乳动物,更优选人的癌症的方法 及其片段,从而通过减少,改善和/或消除癌症作为抗癌剂; 以及通过与用于治疗和/或免疫治疗的免疫治疗剂和/或化学治疗剂共同施用IL-21多肽,多核苷酸,IL-21载体,变体及其片段来治疗和/或预防受试者的癌症的方法。 预防受试者的癌症。
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公开(公告)号:US20050170459A1
公开(公告)日:2005-08-04
申请号:US11052427
申请日:2005-02-07
申请人: Akhilesh Pandey , Katsutoshi Ozaki , Heinz Baumann , Steven Levin , Andrew Farr , Warren Leonard , Harvey Lodish
发明人: Akhilesh Pandey , Katsutoshi Ozaki , Heinz Baumann , Steven Levin , Andrew Farr , Warren Leonard , Harvey Lodish
IPC分类号: A61K38/00 , C07K14/715 , C07H21/04 , C07K16/18 , C12N5/06
CPC分类号: C07K14/7155 , A61K38/00 , C07K2319/30
摘要: The present invention provides Thymic Stromal Lymphopoietin Receptor (TSLPR) polypeptides and nucleic acid molecules encoding the same. The invention also provides selective binding agents, vectors, host cells, and methods for producing TSLPR polypeptides. The invention further provides pharmaceutical compositions and methods for the diagnosis, treatment, amelioration, and/or prevention of diseases, disorders, and conditions associated with TSLPR polypeptides.
摘要翻译: 本发明提供了胸腺基质淋巴细胞生成素受体(TSLPR)多肽和编码其的核酸分子。 本发明还提供选择性结合剂,载体,宿主细胞和用于产生TSLPR多肽的方法。 本发明还提供了用于诊断,治疗,改善和/或预防与TSLPR多肽相关的疾病,病症和病症的药物组合物和方法。
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公开(公告)号:US20070237787A1
公开(公告)日:2007-10-11
申请号:US11762357
申请日:2007-06-13
申请人: Warren Leonard , Akhilesh Pandey , Amin Al-Shami , Rosanne Spolski , John Kelly , Andrea Keane-Myers
发明人: Warren Leonard , Akhilesh Pandey , Amin Al-Shami , Rosanne Spolski , John Kelly , Andrea Keane-Myers
CPC分类号: A61K35/17 , A01K67/0276 , A01K2217/075 , A01K2217/15 , A01K2227/105 , A01K2267/0387 , A61K9/0078 , A61K31/7088 , A61K38/00 , A61K41/00 , A61K45/06 , A61K48/00 , A61K2039/505 , C07K14/5418 , C07K16/244 , A61K2300/00
摘要: Methods are disclosed herein for specifically inducing proliferation of CD4+ T cells. The methods are of use in treating immunodeficiencies, such as an immunodeficiency produced by infection with an immunodeficiency virus, such as infection with a human immunodeficiency virus (HIV). The methods include contacting isolated mammalian CD4+ T cells with an effective amount of a thymic stromal derived lymphopoietin (TSLP) polypeptide or a therapeutically effective amount of nucleic acid encoding the TSLP polypeptide, thereby inducing proliferation of the T cells. Methods are also disclosed for treating an IgE mediated disorder, such as asthma. The methods include administering to a subject a therapeutically effective amount of a TSLP antagonist. Transgenic mice are also disclosed herein. The somatic and germ cells of these mice include a disrupted thymic stromal lymphopoietin receptor (TSLP) gene, the disruption being sufficient to inhibit the interaction of TSLP with its receptor, and a disrupted γc gene, the disruption being sufficient to reduce signaling through the γc. The mice exhibit diminished thymic cellularity. Methods of using these mice for drug screening are also disclosed.
摘要翻译: 本文公开了用于特异性诱导CD4 + T细胞增殖的方法。 该方法可用于治疗免疫缺陷,例如由免疫缺陷病毒感染产生的免疫缺陷,例如人免疫缺陷病毒(HIV)的感染。 所述方法包括使分离的哺乳动物CD4 + T细胞与有效量的胸腺基质衍生的淋巴细胞生成素(TSLP)多肽或治疗有效量的编码TSLP多肽的核酸接触,从而诱导T细胞的增殖。 还公开了用于治疗IgE介导的病症如哮喘的方法。 所述方法包括向受试者施用治疗有效量的TSLP拮抗剂。 本文还公开了转基因小鼠。 这些小鼠的体细胞和生殖细胞包括破坏的胸腺基质淋巴细胞生成素受体(TSLP)基因,破坏足以抑制TSLP与其受体的相互作用,以及破坏的γ基因,破坏 足以减少信号通过伽马。 小鼠表现出胸腺细胞减少。 还公开了将这些小鼠用于药物筛选的方法。
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公开(公告)号:US20060225383A1
公开(公告)日:2006-10-12
申请号:US11101846
申请日:2005-04-08
申请人: William Cobb , Michael Davis , Howitt Smith , Justin Wyatt , Warren Leonard , Darol Foster , Kevin Spicer , Barton Mitchell
发明人: William Cobb , Michael Davis , Howitt Smith , Justin Wyatt , Warren Leonard , Darol Foster , Kevin Spicer , Barton Mitchell
IPC分类号: B65B11/58
CPC分类号: G07F11/44 , A61J7/02 , G07F17/0092
摘要: The present invention relates to an automated system for pharmaceutical singulation, counting and dispensing, whereby a bulk of stored pharmaceutical units are singulated into a single file line for counting and dispensing. With reference to the drawings, the pharmaceutical singulation, counting and dispensing system comprises generally, a deck assembly (A), a cylindrical chamber (B), a rotatable transport ring (C), a plurality of adjustable fingers (D), an adjustable reciprocating member (E), an adjustable rotatable member (F), a counting system (G), a hopper (H), and a control system (I).
摘要翻译: 本发明涉及一种用于药物分离,计数和分配的自动化系统,由此将大量储存的药物单元分割成单个文件管线用于计数和分配。 参考附图,药物分切,计数和分配系统通常包括甲板组件(A),圆柱形腔室(B),可旋转运输环(C),多个可调节手指(D),可调节 往复运动件(E),可调节可旋转件(F),计数系统(G),料斗(H)和控制系统(I)。
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8.发明申请公开(公告)号:US20060057123A1
公开(公告)日:2006-03-16
申请号:US11197221
申请日:2005-08-03
CPC分类号: G01N33/5052 , A61K35/17 , A61K38/20 , A61K2035/124 , A61K2039/5158 , C12N5/0635 , C12N2501/052 , C12N2501/23 , C12N2501/50 , C12N2501/52 , G01N2333/54
摘要: A method is disclosed herein for inducing differentiation of a B cell progenitor into a memory B cells and/or a plasma cell. The method includes contacting a population of cells including a mature B cell or a B cell progenitor with an effective amount of IL-21, and isolating memory B cells or plasma cells. In one embodiment, the B cell progenitor is an immature B cell. A method is also disclosed for enhancing an immune response. The method includes contacting a population of cells including a B cell progenitor with an effective amount of IL-21, and isolating memory B cells or plasma cells. The memory B cells and/or the plasma cell are then introduced into the subject to enhance the immune response. A method is also disclosed for treating a subject with a condition comprising a specific deficiency of at least one of memory B cells and plasma cells. A method is disclosed for identifying an agent with a physiological effect on one or more of a memory B cell and a plasma cell differentiation. A method is also disclosed for identifying agents that inhibit an activity of IL-21. Methods are also disclosed for inducing apoptosis of a B cell and for decreasing the number of B cells. A method is also described for producing a B cell hybridoma.
摘要翻译: 本文公开了一种用于诱导B细胞祖细胞分化为记忆B细胞和/或浆细胞的方法。 该方法包括使包含成熟B细胞或B细胞祖细胞的细胞群与有效量的IL-21接触,并分离记忆B细胞或浆细胞。 在一个实施方案中,B细胞祖细胞是未成熟B细胞。 还公开了一种用于增强免疫应答的方法。 该方法包括使包含B细胞祖细胞的细胞群与有效量的IL-21接触,并分离记忆B细胞或浆细胞。 然后将记忆B细胞和/或浆细胞引入受试者以增强免疫应答。 还公开了一种用于治疗患有包含存储B细胞和浆细胞中的至少一种的特定缺陷的病症的受试者的方法。 公开了用于鉴定对存储B细胞和浆细胞分化中的一种或多种具有生理作用的药剂的方法。 还公开了用于鉴定抑制IL-21活性的试剂的方法。 还公开了诱导B细胞凋亡和减少B细胞数量的方法。 还描述了用于产生B细胞杂交瘤的方法。
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9.发明申请公开(公告)号:US20070003515A1
公开(公告)日:2007-01-04
申请号:US10579988
申请日:2004-11-18
IPC分类号: A61K38/20 , A61K35/14 , G01N33/567
CPC分类号: G01N33/5052 , A61K35/17 , A61K38/20 , A61K2035/124 , A61K2039/5158 , C12N5/0635 , C12N2501/052 , C12N2501/23 , C12N2501/50 , C12N2501/52 , G01N2333/54
摘要: A method is disclosed herein for inducing differentiation of a B cell progenitor into a memory B cells and/or a plasma cell. The method includes contacting a population of cells including a mature B cell or a B cell progenitor with an effective amount of IL-21, and isolating memory B cells or plasma cells. In one embodiment, the B cell progenitor is an immature B cell. A method is also disclosed for enhancing an immune response. The method includes contacting a population of cells including a B cell progenitor with an effective amount of IL-21, and isolating memory B cells or plasma cells. The memory B cells arid/or the plasma cell are then introduced into the subject to enhance the immune response. A method is also disclosed for treating a subject with a condition comprising a specific deficiency of at least one of memory B cells and plasma cells. A method is disclosed for identifying an agent with a physiological effect on one or more of a memory B cell and a plasma cell differentiation. A method is also disclosed for identifying agents that inhibit an activity of IL-21.
摘要翻译: 本文公开了一种用于诱导B细胞祖细胞分化为记忆B细胞和/或浆细胞的方法。 该方法包括使包含成熟B细胞或B细胞祖细胞的细胞群与有效量的IL-21接触,并分离记忆B细胞或浆细胞。 在一个实施方案中,B细胞祖细胞是未成熟B细胞。 还公开了一种用于增强免疫应答的方法。 该方法包括使包含B细胞祖细胞的细胞群与有效量的IL-21接触,并分离记忆B细胞或浆细胞。 然后将记忆B细胞和/或浆细胞引入受试者以增强免疫应答。 还公开了一种用于治疗患有包含存储B细胞和浆细胞中的至少一种的特定缺陷的病症的受试者的方法。 公开了用于鉴定对存储B细胞和浆细胞分化中的一种或多种具有生理作用的药剂的方法。 还公开了用于鉴定抑制IL-21活性的试剂的方法。
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公开(公告)号:US20050271668A1
公开(公告)日:2005-12-08
申请号:US11195197
申请日:2005-08-01
申请人: John O'Shea , Warren Leonard , James Johnston , Sarah Russell , Daniel McVicar , Masaru Kawamura
发明人: John O'Shea , Warren Leonard , James Johnston , Sarah Russell , Daniel McVicar , Masaru Kawamura
IPC分类号: A61K39/395 , A61K48/00 , C07H21/04 , C07K16/40 , C12N9/12
CPC分类号: C12N9/1205 , A61K48/00 , C07K16/40
摘要: An isolated polynucleotide encodes JAK-3 protein. JAK-3 protein is a protein tyrosine kinase having a molecular weight of approximately 125 kDa which has tandem non-identical catalytic domains, lacks SH2 or SH3 domains, and is expressed in NK cells and stimulated or transformed T cells, but not in resting T cells. The protein itself and antibodies to this protein are also presented. Further, methods of identifying therapeutic agents for modulating the immune system make use of the foregoing.
摘要翻译: 分离的多核苷酸编码JAK-3蛋白。 JAK-3蛋白是具有约125kDa分子量的蛋白酪氨酸激酶,其具有串联的不相同的催化结构域,缺少SH2或SH3结构域,并且在NK细胞和刺激或转化的T细胞中表达,但不在休息T 细胞。 蛋白质本身和对该蛋白质的抗体也被提出。 此外,鉴定用于调节免疫系统的治疗剂的方法利用上述。
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