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公开(公告)号:US08658765B2
公开(公告)日:2014-02-25
申请号:US12982827
申请日:2010-12-30
Applicant: David W. Martin, Jr. , Steven R. Williams
Inventor: David W. Martin, Jr. , Steven R. Williams
CPC classification number: C07K14/70539 , A61K38/1774 , C07K2319/33 , Y02A50/389 , Y02A50/393
Abstract: This invention describes soluble, monovalent, non-natural protein molecules that can activate NK cells and certain T-cells to attack specific cellular target cells by attaching the NKG2D-binding portions of monovalent MICA or MICB protein, i.e. their α1-α2 platform domain, to the intended target cell specifically. The α1-α2 domain is contiguous with a heterologous α3 domain that has been genetically modified to bind directly or indirectly to the extracellular aspect of the target cell, thereby serving as the targeting domain. The genetic modification to create a non-natural and non-terminal targeting motif within the α3 domain can include a portion of an antibody, another protein molecule or portion thereof, a peptide, or a non-natural, modified α3 domain of a MIC protein.
Abstract translation: 本发明描述了通过连接单价MICA或MICB蛋白(即它们的α1-α2平台结构域)的NKG2D结合部分可以激活NK细胞和某些T细胞以攻击特定细胞靶细胞的可溶性,一价,非天然蛋白质分子, 具体到目的细胞。 α1-α2结构域与经过遗传修饰的异源α3结构域连续,直接或间接地结合靶细胞的细胞外区域,从而作为靶向结构域。 在α3结构域内产生非天然和非末端靶向基序的遗传修饰可包括MIC蛋白的一部分抗体,另一蛋白质分子或其部分,肽或非天然修饰的α3结构域 。
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公开(公告)号:US20100261258A1
公开(公告)日:2010-10-14
申请号:US12701431
申请日:2010-02-05
Applicant: Dean M. Scholl , Steven R. Williams
Inventor: Dean M. Scholl , Steven R. Williams
IPC: C12N1/21
CPC classification number: C07K14/21 , C07K2319/35 , C07K2319/74
Abstract: Modified forms of naturally occurring bacteriocins, such as the R-type pyocins of Pseudomonas aeruginosa, are disclosed as are methods for producing them in GRAS organisms. The bacteriocins are modified at the ends of their tail fibers in a region responsible for binding specificity and affinity to their cognate binding partners, or receptors, such as those on the surface of bacteria. Methods for the use of the modified bacteriocins, such as to bind receptors, including virulence or fitness factors, on the surfaces of bacteria, are also described.
Abstract translation: 公开了天然存在的细菌素的修饰形式,例如绿脓假单胞菌的R型py霉素,作为在GRAS生物体中生产它们的方法。 细菌素在其尾纤维的末端被修饰,负责对其同源结合配偶体或受体(例如细菌表面上的那些)的结合特异性和亲和力。 还描述了在细菌表面上使用修饰的细菌素,例如结合受体(包括毒力或适应因子)的方法。
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公开(公告)号:US20080113406A1
公开(公告)日:2008-05-15
申请号:US11748432
申请日:2007-05-14
Applicant: David W. Martin , Andrew C. Jamieson , Dean M. Scholl , Steven R. Williams
Inventor: David W. Martin , Andrew C. Jamieson , Dean M. Scholl , Steven R. Williams
IPC: C07K14/195 , C12N1/21 , C07H21/04 , C12P21/06 , C12N15/74
CPC classification number: C07K14/21 , C07K2319/35 , C07K2319/74
Abstract: Modified forms of naturally occurring bacteriocins, such as the R-type pyocins of Pseudomonas aeruginosa, are disclosed. The bacteriocins are modified at the ends of their tail fibers in a region responsible for binding specificity and affinity to their cognate binding partners, or receptors, such as those on the surface of bacteria. Methods for the use of the modified bacteriocins, such as to bind receptors, including virulence or fitness factors, on the surfaces of bacteria, are also described.
Abstract translation: 公开了天然存在的细菌素的修饰形式,例如铜绿假单胞菌的R型py虫。 细菌素在其尾纤维的末端被修饰,负责对其同源结合配偶体或受体(例如细菌表面上的那些)的结合特异性和亲和力。 还描述了在细菌表面上使用修饰的细菌素,例如结合受体(包括毒力或适应因子)的方法。
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公开(公告)号:US20140302072A1
公开(公告)日:2014-10-09
申请号:US14311130
申请日:2014-06-20
Applicant: David W. MARTIN, JR. , Steven R. Williams
Inventor: David W. MARTIN, JR. , Steven R. Williams
IPC: C07K14/47
CPC classification number: C07K14/473 , A61K38/00 , C07K14/70539 , C07K2318/00 , C07K2319/33 , Y02A50/389 , Y02A50/393
Abstract: This invention describes soluble, monovalent, non-natural protein molecules that can activate NK cells and certain T-cells to attack specific cellular target cells by attaching the NKG2D-binding portions of monovalent MICA or MICB protein, i.e. their α1-α2 platform domain, to the intended target cell specifically. The α1-α2 domain is contiguous with a heterologous α3 domain that has been genetically modified to bind directly or indirectly to the extracellular aspect of the target cell, thereby serving as the targeting domain. The genetic modification to create a non-natural and non-terminal targeting motif within the α3 domain can include a portion of an antibody, another protein molecule or portion thereof, a peptide, or a non-natural, modified α3 domain of a MIC protein.
Abstract translation: 本发明描述了通过连接单价MICA或MICB蛋白(即它们的α1-α2平台结构域)的NKG2D结合部分可以激活NK细胞和某些T细胞以攻击特异性细胞靶细胞的可溶性,一价,非天然蛋白质分子, 具体到目的细胞。 α1-α2结构域与已经被遗传修饰的异源α3结构域连续,直接或间接地结合到靶细胞的细胞外方面,从而作为靶向结构域。 在α3结构域内产生非天然和非末端靶向基序的遗传修饰可以包括MIC蛋白质的一部分抗体,另一蛋白质分子或其部分,肽或非天然修饰的α3结构域 。
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公开(公告)号:US08206971B2
公开(公告)日:2012-06-26
申请号:US12701431
申请日:2010-02-05
Applicant: Dean M. Scholl , Steven R. Williams
Inventor: Dean M. Scholl , Steven R. Williams
IPC: C12N1/20
CPC classification number: C07K14/21 , C07K2319/35 , C07K2319/74
Abstract: Modified forms of naturally occurring bacteriocins, such as the R-type pyocins of Pseudomonas aeruginosa, are disclosed as are methods for producing them in GRAS organisms. The bacteriocins are modified at the ends of their tail fibers in a region responsible for binding specificity and affinity to their cognate binding partners, or receptors, such as those on the surface of bacteria. Methods for the use of the modified bacteriocins, such as to bind receptors, including virulence or fitness factors, on the surfaces of bacteria, are also described.
Abstract translation: 公开了天然存在的细菌素的修饰形式,例如绿脓假单胞菌的R型py霉素,作为在GRAS生物体中生产它们的方法。 细菌素在其尾纤维的末端被修饰,负责对其同源结合配偶体或受体(例如细菌表面上的那些)的结合特异性和亲和力。 还描述了在细菌表面上使用修饰的细菌素,例如结合受体(包括毒力或适应因子)的方法。
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Patent Agency Ranking
公开(公告)号:US20110311561A1
公开(公告)日:2011-12-22
申请号:US13176601
申请日:2011-07-05
Applicant: David W. Martin, JR. , Steven R. Williams
Inventor: David W. Martin, JR. , Steven R. Williams
CPC classification number: C07K14/473 , A61K38/00 , C07K14/70539 , C07K2318/00 , C07K2319/33 , Y02A50/389 , Y02A50/393
Abstract: This invention describes soluble, monovalent, non-natural protein molecules that can activate NK cells and certain T-cells to attack specific cellular target cells by attaching the NKG2D-binding portions of monovalent MICA or MICB protein, i.e. their α1-α2 platform domain, to the intended target cell specifically. The α1-α2 domain is contiguous with a heterologous α3 domain that has been genetically modified to bind directly or indirectly to the extracellular aspect of the target cell, thereby serving as the targeting domain. The genetic modification to create a non-natural and non-terminal targeting motif within the α3 domain can include a portion of an antibody, another protein molecule or portion thereof, a peptide, or a non-natural, modified α3 domain of a MIC protein.
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公开(公告)号:US08796420B2
公开(公告)日:2014-08-05
申请号:US13176601
申请日:2011-07-05
Applicant: David W. Martin, Jr. , Steven R. Williams
Inventor: David W. Martin, Jr. , Steven R. Williams
IPC: A61K38/16 , C07K16/00 , A01N63/00 , C07K19/00 , C12N5/0783
CPC classification number: C07K14/473 , A61K38/00 , C07K14/70539 , C07K2318/00 , C07K2319/33 , Y02A50/389 , Y02A50/393
Abstract: This invention describes soluble, monovalent, non-natural protein molecules that can activate NK cells and certain T-cells to attack specific cellular target cells by attaching the NKG2D-binding portions of monovalent MICA or MICB protein, i.e. their α1-α2 platform domain, to the intended target cell specifically. The α1-α2 domain is contiguous with a heterologous α3 domain that has been genetically modified to bind directly or indirectly to the extracellular aspect of the target cell, thereby serving as the targeting domain. The genetic modification to create a non-natural and non-terminal targeting motif within the α3 domain can include a portion of an antibody, another protein molecule or portion thereof, a peptide, or a non-natural, modified α3 domain of a MIC protein.
Abstract translation: 本发明描述了通过连接单价MICA或MICB蛋白(即它们的α1-α2平台结构域)的NKG2D结合部分可以激活NK细胞和某些T细胞以攻击特异性细胞靶细胞的可溶性,一价,非天然蛋白质分子, 具体到目的细胞。 α1-α2结构域与已经被遗传修饰的异源α3结构域连续,直接或间接地结合到靶细胞的细胞外方面,从而作为靶向结构域。 在α3结构域内产生非天然和非末端靶向基序的遗传修饰可以包括MIC蛋白质的一部分抗体,另一蛋白质分子或其部分,肽或非天然修饰的α3结构域 。
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公开(公告)号:US20080171376A1
公开(公告)日:2008-07-17
申请号:US11929867
申请日:2007-10-30
Applicant: Dean M. SCHOLL , Steven R. WILLIAMS
Inventor: Dean M. SCHOLL , Steven R. WILLIAMS
CPC classification number: C07K14/21 , C07K2319/35 , C07K2319/74
Abstract: Modified forms of naturally occurring bacteriocins, such as the R-type pyocins of Pseudomonas aeruginosa, are disclosed as are methods for producing them in GRAS organisms. The bacteriocins are modified at the ends of their tail fibers in a region responsible for binding specificity and affinity to their cognate binding partners, or receptors, such as those on the surface of bacteria. Methods for the use of the modified bacteriocins, such as to bind receptors, including virulence or fitness factors, on the surfaces of bacteria, are also described.
Abstract translation: 公开了天然存在的细菌素的修饰形式,例如绿脓假单胞菌的R型py霉素,作为在GRAS生物体中生产它们的方法。 细菌素在其尾纤维的末端被修饰,负责对其同源结合配偶体或受体(例如细菌表面上的那些)的结合特异性和亲和力。 还描述了在细菌表面上使用修饰的细菌素,例如结合受体(包括毒力或适应因子)的方法。
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9.发明授权Homologous recombination for universal donor cells and chimeric mammalian hosts 失效用于通用供体细胞和嵌合哺乳动物宿主的同源重组公开(公告)号:US06514752B1
公开(公告)日:2003-02-04
申请号:US08443613
申请日:1995-05-18
Applicant: Raju Kucherlapati , Beverly H. Koller , Oliver Smithies , Robert B. Dubridge , Gary Greenburg , Daniel J. Capon , Steven R. Williams , Mariona Lourdes Arbones De Rafael
Inventor: Raju Kucherlapati , Beverly H. Koller , Oliver Smithies , Robert B. Dubridge , Gary Greenburg , Daniel J. Capon , Steven R. Williams , Mariona Lourdes Arbones De Rafael
IPC: C12N1574
CPC classification number: A01K67/0271 , A01K67/0275 , A01K67/0276 , A01K2207/15 , A01K2217/00 , A01K2217/075 , A01K2227/105 , A01K2267/025 , A01K2267/03 , A01K2267/0381 , C07K14/70539 , C12N15/00 , C12N15/8509
Abstract: Homologous recombination is employed to inactivate genes, particularly genes associated with MHC antigens. Particularly, the &bgr;2-microglobulin gene is inactivated for reducing or eliminating the expression of functional Class I MHC antigens. The resulting cells may be used as universal donor cells. In addition, embryonic stem cells may be modified by homologous recombination for use in producing chimeric or transgenic mammalian hosts, which may be used as source of universal donor organs, or as models for drug and transplantation therapies. Methods for homologous recombination in non-transformed mammalian somatic cells are also described.
Abstract translation: 同源重组用于灭活基因,特别是与MHC抗原相关的基因。 特别地,β2-微球蛋白基因被灭活以减少或消除功能性I类MHC抗原的表达。 所得细胞可用作通用供体细胞。 此外,胚胎干细胞可以通过同源重组来修饰,用于产生嵌合或转基因哺乳动物宿主,其可以用作通用供体器官的来源,或作为药物和移植疗法的模型。 还描述了在非转化的哺乳动物体细胞中同源重组的方法。
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公开(公告)号:US6139835A
公开(公告)日:2000-10-31
申请号:US443647
申请日:1995-05-18
Applicant: Raju Kucherlapati , Beverly H. Koller , Oliver Smithies , Robert B. Dubridge , Gary Greenburg , Daniel J. Capon , Steven R. Williams , Mariona Lourdes Arbones De Rafael
Inventor: Raju Kucherlapati , Beverly H. Koller , Oliver Smithies , Robert B. Dubridge , Gary Greenburg , Daniel J. Capon , Steven R. Williams , Mariona Lourdes Arbones De Rafael
IPC: A01K67/027 , A61K35/12 , A61K38/21 , A61K45/00 , C07H21/04 , C07K14/74 , C12N5/02 , C12N5/10 , C12N15/00 , C12N15/09 , C12N15/85 , C12Q1/68 , G01N33/53 , C12N15/63
CPC classification number: A01K67/0271 , A01K67/0275 , A01K67/0276 , C07K14/70539 , C12N15/00 , C12N15/8509 , A01K2207/15 , A01K2217/00 , A01K2217/075 , A01K2227/105 , A01K2267/025 , A01K2267/03 , A01K2267/0381
Abstract: Homologous recombination is employed to inactivate genes, particularly genes associated with MHC antigens. Particularly, the .beta..sub.2- microglobulin gene is inactivated for reducing or eliminating the expression of functional Class I MHC antigens. The resulting cells may be used as allogeneic donor cells. Methods for homologous recombination in non-transformed mammalian somatic cells are also described.
Abstract translation: 同源重组用于灭活基因,特别是与MHC抗原相关的基因。 特别地,β2-微球蛋白基因被灭活以减少或消除功能性I类MHC抗原的表达。 所得细胞可用作同种异体供体细胞。 还描述了在非转化的哺乳动物体细胞中同源重组的方法。
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