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公开(公告)号:US20060019309A1
公开(公告)日:2006-01-26
申请号:US11068936
申请日:2005-02-28
申请人: Shuguang Zhang , Alexander Rich , Lin Yan , George Whitesides
发明人: Shuguang Zhang , Alexander Rich , Lin Yan , George Whitesides
CPC分类号: B82Y30/00 , B01J19/0046 , B01J2219/00382 , B01J2219/00605 , B01J2219/00612 , B01J2219/00617 , B01J2219/00619 , B01J2219/00626 , B01J2219/0063 , B01J2219/00635 , B01J2219/00637 , B01J2219/00659 , B01J2219/00725 , B01J2219/00743 , B82Y5/00 , B82Y10/00 , B82Y40/00 , C07K2/00 , C07K7/08 , C07K17/14 , C12N5/0068 , C12N2535/10 , C40B40/10 , C40B60/14 , G01N33/54353 , G01N2610/00 , G03F7/0002 , G03F7/165
摘要: This invention describes self assembled monolayers (SAMs) manufactured by imprinting reactive peptides onto solid supports. The invention further relates to methods of preparing and using these improved SAMs.
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公开(公告)号:US06368877B1
公开(公告)日:2002-04-09
申请号:US08882415
申请日:1997-06-25
申请人: Shuguang Zhang , Alexander Rich , Lin Yan , George Whitesides
发明人: Shuguang Zhang , Alexander Rich , Lin Yan , George Whitesides
IPC分类号: G01N33552
CPC分类号: B82Y30/00 , B01J19/0046 , B01J2219/00382 , B01J2219/00605 , B01J2219/00612 , B01J2219/00617 , B01J2219/00619 , B01J2219/00626 , B01J2219/0063 , B01J2219/00635 , B01J2219/00637 , B01J2219/00659 , B01J2219/00725 , B01J2219/00743 , B82Y5/00 , B82Y10/00 , B82Y40/00 , C07K2/00 , C07K7/08 , C07K17/14 , C12N5/0068 , C12N2535/10 , C40B40/10 , C40B60/14 , G01N33/54353 , G01N2610/00 , G03F7/0002 , G03F7/165
摘要: This invention describes self assembled monolayers (SAMs) manufactured by imprinting reactive peptides onto solid supports. The invention further relates to methods of preparing and using these improved SAMs.
摘要翻译: 本发明描述了通过将反应性肽印迹到固体支持物上制造的自组装单层(SAM)。 本发明还涉及制备和使用这些改进的SAM的方法。
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3.发明申请Stable macroscopic membranes formed by self-assembly of amphiphilic peptides and uses therefor 审中-公开通过两亲肽的自组装形成稳定的宏观膜并用于其公开(公告)号:US20070190603A1
公开(公告)日:2007-08-16
申请号:US11512753
申请日:2006-08-29
申请人: Todd Holmes , Shuguang Zhang , Alexander Rich , C. DiPersio , Curtis Lockshin
发明人: Todd Holmes , Shuguang Zhang , Alexander Rich , C. DiPersio , Curtis Lockshin
CPC分类号: C07K7/08 , A61K9/009 , C07K5/0815 , C07K7/06 , C07K14/001 , C07K14/395 , C12N5/0068 , C12N2533/30 , C12N2533/50
摘要: Described herein is the self-assembly of amphiphilic peptides, i.e., peptides with alternating hydrophobic and hydrophilic residues, into macroscopic membranes. The membrane-forming peptides are greater than 12 amino acids in length, and preferably at least 16 amino acids, are complementary and are structurally compatible. Specifically, two peptides, (AEAEAKAK)2 (ARARADAD)2, were shown to self-assemble into macroscopic membranes. Conditions under which the peptides self-assemble into macroscopic membranes and methods for producing the membranes are also described. The macroscopic membranes have several interesting properties: they are stable in aqueous solution, serum, and ethanol, are highly resistant to heat, alkaline and acidic pH, chemical denaturants, and proteolytic digestion, and are non-cytotoxic. The membranes are potentially useful in biomaterial applications such as slow-diffusion drug delivery systems, artificial skin, and separation matrices, and as experimental models for Alzheimer's disease and scrapie infection. The sequence of the peptide, EAK16, was derived from a putative Z-DNA binding protein from yeast, called zuotin. The cloning and characterization of the ZUO1 gene are also described.
摘要翻译: 这里描述的是将两亲肽,即具有交替疏水和亲水残基的肽自组装成宏观膜。 成膜肽长度大于12个氨基酸,优选至少16个氨基酸是互补的并且在结构上相容。 具体来说,显示两种肽(AEAEAKAK)2(ARARADAD)2 N自组装成宏观膜。 还描述了肽自组装成宏观膜的条件和制备膜的方法。 肉眼膜具有几个有趣的性质:它们在水溶液,血清和乙醇中稳定,对热,碱性和酸性pH,化学变性剂和蛋白水解消化具有高度抗性,并且是非细胞毒性的。 该膜可用于生物材料应用,如慢扩散药物递送系统,人造皮肤和分离基质,以及阿尔茨海默病和瘙痒病感染的实验模型。 肽EAK16的序列衍生自称为佐酮的来自酵母的推定的Z-DNA结合蛋白。 还描述了ZUO1基因的克隆和表征。
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4.发明授权Stable macroscopic membranes formed by self-assembly of amphiphilic peptides and uses therefor 失效通过两亲肽的自组装形成稳定的宏观膜并用于其公开(公告)号:US06548630B1
公开(公告)日:2003-04-15
申请号:US08898300
申请日:1997-07-22
申请人: Shuguang Zhang , Curtis Lockshin , Alexander Rich , Todd Holmes
发明人: Shuguang Zhang , Curtis Lockshin , Alexander Rich , Todd Holmes
IPC分类号: C07K700
CPC分类号: C07K7/08 , A61K9/009 , C07K14/001 , C07K14/395 , C12N5/0068 , C12N2533/30 , C12N2533/50
摘要: Described herein is the self-assembly of amphiphilic peptides, i.e., peptides with alternating hydrophobic and hydrophilic residues, into macroscopic membranes. The membrane-forming peptides are greater than 12 amino acids in length, and preferably at least 16 amino acids, are complementary and are structurally compatible. Specifically, two peptides, (AEAEAKAK)2 (ARARADAD)2, were shown to self-assemble into macroscopic membranes. Conditions under which the peptides self-assemble into macroscopic membranes and methods for producing the membranes are also described. The macroscopic membranes have several interesting properties: they are stable in aqueous solution, serum, and ethanol, are highly resistant to heat, alkaline and acidic pH, chemical denaturants, and proteolytic digestion, and are non-cytotoxic. The membranes are potentially useful in biomaterial applications such as slow-diffusion drug delivery systems, artificial skin, and separation matrices, and as experimental models for Alzheimer's disease and scrapie infection. The sequence of the peptide, EAK16, was derived from a putative Z-DNA binding protein from yeast, called zuotin. The cloning and characterization of the ZUO1 gene are also described.
摘要翻译: 这里描述的是将两亲肽,即具有交替疏水和亲水残基的肽自组装成宏观膜。 成膜肽长度大于12个氨基酸,优选至少16个氨基酸是互补的并且在结构上相容。 具体来说,显示两种肽(AEAEAKAK)2(ARARADAD)2自组装成宏观膜。 还描述了肽自组装成宏观膜的条件和制备膜的方法。 肉眼膜具有几个有趣的性质:它们在水溶液,血清和乙醇中稳定,对热,碱性和酸性pH,化学变性剂和蛋白水解消化具有高度抗性,并且是非细胞毒性的。 该膜可用于生物材料应用,如慢扩散药物递送系统,人造皮肤和分离基质,以及阿尔茨海默病和瘙痒病感染的实验模型。 肽EAK16的序列衍生自称为佐酮的来自酵母的推定的Z-DNA结合蛋白。 还描述了ZUO1基因的克隆和表征。
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5.发明授权Stable macroscopic membranes formed by self-assembly of amphiphilic peptides and uses therefor 失效通过两亲肽的自组装形成稳定的宏观膜并用于其
公开(公告)号:US5670483A
公开(公告)日:1997-09-23
申请号:US346849
申请日:1994-11-30
申请人: Shuguang Zhang , Curtis Lockshin , Alexander Rich , Todd Holmes
发明人: Shuguang Zhang , Curtis Lockshin , Alexander Rich , Todd Holmes
IPC分类号: A61K9/00 , C07K7/08 , C07K14/00 , C07K14/395 , C12N5/00 , C12N5/02 , A61K7/08 , A61K14/00 , C07K38/10 , C07K38/16
CPC分类号: C07K7/08 , C07K14/001 , C07K14/395 , C12N5/0068 , A61K9/009 , C12N2533/30 , C12N2533/50
摘要: Described herein is the self-assembly of amphiphilic peptides, i.e., peptides with alternating hydrophobic and hydrophilic residues, into macroscopic membranes. The membrane-forming peptides are greater than 12 amino acids in length, and preferably at least 16 amino acids, are complementary and are structurally compatible. Specifically, two peptides, (AEAEAKAK).sub.2 (ARARADAD).sub.2, were shown to self-assemble into macroscopic membranes. Conditions under which the peptides self-assemble into macroscopic membranes and methods for producing the membranes are also described. The macroscopic membranes have several interesting properties: they are stable in aqueous solution, serum, and ethanol, are highly resistant to heat, alkaline and acidic pH, chemical denaturants, and proteolytic digestion, and are non-cytotoxic. The membranes are potentially useful in biomaterial applications such as slow-diffusion drug delivery systems, artificial skin, and separation matrices, and as experimental models for Alzheimer's disease and scrapie infection. The sequence of the peptide, EAK16, was derived from a putative Z-DNA binding protein from yeast, called zuotin. The cloning and characterization of the ZUO1 gene are also described.
摘要翻译: 这里描述的是将两亲肽,即具有交替疏水和亲水残基的肽自组装成宏观膜。 成膜肽长度大于12个氨基酸,优选至少16个氨基酸是互补的并且在结构上相容。 具体来说,显示两种肽(AEAEAKAK)2(ARARADAD)2自组装成宏观膜。 还描述了肽自组装成宏观膜的条件和制备膜的方法。 肉眼膜具有几个有趣的性质:它们在水溶液,血清和乙醇中稳定,对热,碱性和酸性pH,化学变性剂和蛋白水解消化具有高度抗性,并且是非细胞毒性的。 该膜可用于生物材料应用,如慢扩散药物递送系统,人造皮肤和分离基质,以及阿尔茨海默病和瘙痒病感染的实验模型。 肽EAK16的序列衍生自称为佐酮的来自酵母的推定的Z-DNA结合蛋白。 还描述了ZUO1基因的克隆和表征。
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6.发明申请公开(公告)号:US20120252719A1
公开(公告)日:2012-10-04
申请号:US13403725
申请日:2012-02-23
IPC分类号: A61K38/17 , G01N21/55 , C07K14/705 , C07K1/107 , A61P9/00 , A61P9/12 , A61P11/06 , G01N25/00 , A61P25/16
CPC分类号: C07K14/705 , A61K38/00 , A61K38/17 , A61K38/177 , A61K38/1793 , C07K14/7158 , G01N33/6863
摘要: The present invention is directed to water-soluble membrane proteins, methods for the preparation thereof and methods of use thereof.
摘要翻译: 本发明涉及水溶性膜蛋白,其制备方法及其使用方法。
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7.发明授权
公开(公告)号:US5955343A
公开(公告)日:1999-09-21
申请号:US293284
申请日:1994-08-22
CPC分类号: C07K7/08 , C07K14/001 , C07K14/395 , C07K5/0815 , C07K7/06 , C12N5/0068 , A61K9/009 , C12N2533/30 , C12N2533/50
摘要: Described herein is the self-assembly of amphiphilic peptides, i.e., peptides with alternating hydrophobic and hydrophilic residues, into macroscopic membranes. The membrane-forming peptides are greater than 12 amino acids in length, and preferably at least 16 amino acids, are complementary and are structurally compatible. Specifically, two peptides, (AEAEAKAK).sub.2 (ARARADAD).sub.2, were shown to self-assemble into macroscopic membranes. Conditions under which the peptides self-assemble into macroscopic membranes and methods for producing the membranes are also described. The macroscopic membranes have several interesting properties: they are stable in aqueous solution, serum, and ethanol, are highly resistant to heat, alkaline and acidic pH, chemical denaturants, and proteolytic digestion, and are non-cytotoxic. The membranes are potentially useful in biomaterial applications such as slow-diffusion drug delivery systems, artificial skin, and separation matrices, and as experimental models for Alzheimer's disease and scrapie infection. The sequence of the peptide, EAK16, was derived from a putative Z-DNA binding protein from yeast, called zuotin. The cloning and characterization of the ZUO1 gene are also described.
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8.发明授权Stable macroscopic membranes formed by self-assembly of amphiphilic peptides and uses therefor 失效通过两亲肽的自组装形成稳定的宏观膜并用于其公开(公告)号:US07098028B2
公开(公告)日:2006-08-29
申请号:US10390472
申请日:2003-03-17
CPC分类号: C07K7/08 , A61K9/009 , C07K5/0815 , C07K7/06 , C07K14/001 , C07K14/395 , C12N5/0068 , C12N2533/30 , C12N2533/50
摘要: Described herein is the self-assembly of amphiphilic peptides, i.e., peptides with alternating hydrophobic and hydrophilic residues, into macroscopic membranes. The membrane-forming peptides are greater than 12 amino acids in length, and preferably at least 16 amino acids, are complementary and are structurally compatible. Specifically, two peptides, (AEAEAKAK)2 (ARARADAD)2, were shown to self-assemble into macroscopic membranes. Conditions under which the peptides self-assemble into macroscopic membranes and methods for producing the membranes are also described. The macroscopic membranes have several interesting properties: they are stable in aqueous solution, serum, and ethanol, are highly resistant to heat, alkaline and acidic pH, chemical denaturants, and proteolytic digestion, and are non-cytotoxic. The membranes are potentially useful in biomaterial applications such as slow-diffusion drug delivery systems, artificial skin, and separation matrices, and as experimental models for Alzheimer's disease and scrapie infection. The sequence of the peptide, EAK16, was derived from a putative Z-DNA binding protein from yeast, called zuotin. The cloning and characterization of the ZUO1 gene are also described.
摘要翻译: 这里描述的是将两亲肽,即具有交替疏水和亲水残基的肽自组装成宏观膜。 成膜肽长度大于12个氨基酸,优选至少16个氨基酸是互补的并且在结构上相容。 具体来说,显示两种肽(AEAEAKAK)2(ARARADAD)2 N自组装成宏观膜。 还描述了肽自组装成宏观膜的条件和制备膜的方法。 肉眼膜具有几个有趣的性质:它们在水溶液,血清和乙醇中稳定,对热,碱性和酸性pH,化学变性剂和蛋白水解消化具有高度抗性,并且是非细胞毒性的。 该膜可用于生物材料应用,如慢扩散药物递送系统,人造皮肤和分离基质,以及阿尔茨海默病和瘙痒病感染的实验模型。 肽EAK16的序列衍生自称为佐酮的来自酵母的推定的Z-DNA结合蛋白。 还描述了ZUO1基因的克隆和表征。
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9.发明授权公开(公告)号:US08637452B2
公开(公告)日:2014-01-28
申请号:US13403725
申请日:2012-02-23
CPC分类号: C07K14/705 , A61K38/00 , A61K38/17 , A61K38/177 , A61K38/1793 , C07K14/7158 , G01N33/6863
摘要: The present invention is directed to water-soluble membrane proteins, methods for the preparation thereof and methods of use thereof.
摘要翻译: 本发明涉及水溶性膜蛋白,其制备方法及其使用方法。
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10.发明授权Stable macroscopic membranes formed by self-assembly of amphiphilic peptides and uses therefor 失效通过两亲肽的自组装形成稳定的宏观膜并用于其公开(公告)号:US06800481B1
公开(公告)日:2004-10-05
申请号:US08824513
申请日:1997-03-26
IPC分类号: C12N502
CPC分类号: C07K7/08 , A61K9/009 , C07K5/0815 , C07K7/06 , C07K14/001 , C07K14/395 , C12N5/0068 , C12N2533/30 , C12N2533/50
摘要: Described herein is the self-assembly of amphiphilic peptides, i.e., peptides with alternating hydrophobic and hydrophilic residues, into macroscopic membranes. The membrane-forming peptides are greater than 12 amino acids in length, and preferably at least 16 amino acids, are complementary and are structurally compatible. Specifically, two peptides, (AEAEAKAK)2 (ARARADAD)2, were shown to self-assemble into macroscopic membranes. Conditions under which the peptides self-assemble into macroscopic membranes and methods for producing the membranes are also described. The macroscopic membranes have several interesting properties: they are stable in aqueous solution, serum, and ethanol, are highly resistant to heat, alkaline and acidic pH, chemical denaturants, and proteolytic digestion, and are non-cytotoxic. The membranes are potentially useful in biomaterial applications such as slow-diffusion drug delivery systems, artificial skin, and separation matrices, and as experimental models for Alzheimer's disease and scrapie infection. The sequence of the peptide, EAK16, was derived from a putative Z-DNA binding protein from yeast, called zuotin. The cloning and characterization of the ZUO1 gene are also described.
摘要翻译: 这里描述的是将两亲肽,即具有交替疏水和亲水残基的肽自组装成宏观膜。 成膜肽长度大于12个氨基酸,优选至少16个氨基酸是互补的并且在结构上相容。 具体来说,显示两种肽(AEAEAKAK)2(ARARADAD)2自组装成宏观膜。 还描述了肽自组装成宏观膜的条件和制备膜的方法。 肉眼膜具有几个有趣的性质:它们在水溶液,血清和乙醇中稳定,对热,碱性和酸性pH,化学变性剂和蛋白水解消化具有高度抗性,并且是非细胞毒性的。 该膜可用于生物材料应用,如慢扩散药物递送系统,人造皮肤和分离基质,以及阿尔茨海默病和瘙痒病感染的实验模型。 肽EAK16的序列衍生自称为佐酮的来自酵母的推定的Z-DNA结合蛋白。 还描述了ZUO1基因的克隆和表征。
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