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公开(公告)号:US20090130762A1
公开(公告)日:2009-05-21
申请号:US11974958
申请日:2007-10-17
申请人: Xavier Paliard , Michael Houghton , Mark Selby
发明人: Xavier Paliard , Michael Houghton , Mark Selby
CPC分类号: C07K14/005 , A61K48/00 , A61K2039/53 , C07K2319/00 , C12N2770/24222
摘要: The invention provides a method of activating hepatitis C virus (HCV)-specific T cells, including CD4+ and CD8+ T cells. HCV-specific T cells are activated using fusion proteins comprising HCV NS3, NS4, NS5a, and NS5b polypeptides, polynucleotides encoding such fusion proteins, or polypeptide or polynucleotide compositions containing the individual components of these fusions. The method can be used in model systems to develop HCV-specific immunogenic compositions, as well as to immunize a mammal against HCV.
摘要翻译: 本发明提供一种激活丙型肝炎病毒(HCV)特异性T细胞,包括CD4 +和CD8 + T细胞的方法。 使用包含HCV NS3,NS4,NS5a和NS5b多肽的融合蛋白,编码这种融合蛋白的多核苷酸或含有这些融合物的各个组分的多肽或多核苷酸组合物来激活HCV特异性T细胞。 该方法可以在模型系统中用于开发HCV特异性免疫原性组合物,以及免疫哺乳动物抗HCV。
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公开(公告)号:US20090098153A1
公开(公告)日:2009-04-16
申请号:US12231351
申请日:2008-09-02
申请人: Michael Houghton , Steve Coates , Mark Selby , Xavier Paliard
发明人: Michael Houghton , Steve Coates , Mark Selby , Xavier Paliard
IPC分类号: A61K39/00
CPC分类号: C07K14/005 , A61K48/00 , A61K2039/53 , C07K2319/00 , C12N2770/24222
摘要: The invention provides a method of activating hepatitis C virus (HCV)-specific T cells, including CD4+ and CD8+ T cells. HCV-specific T cells are activated using fusion proteins comprising HCV NS3, NS4, NS5a, and NS5b polypeptides, polynucleotides encoding such fusion proteins, or polypeptide or polynucleotide compositions containing the individual components of these fusions. The method can be used in model systems to develop HCV-specific immunogenic compositions, as well as to immunize a mammal against HCV.
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公开(公告)号:US06562346B1
公开(公告)日:2003-05-13
申请号:US09698874
申请日:2000-10-27
申请人: Xavier Paliard , Michael Houghton , Mark Selby
发明人: Xavier Paliard , Michael Houghton , Mark Selby
IPC分类号: A61K3929
CPC分类号: C07K14/005 , A61K48/00 , A61K2039/53 , C07K2319/00 , C12N2770/24222
摘要: The invention provides a method of activating hepatitis C virus (HCV)-specific T cells, including CD4+ and CD8+ T cells. HCV-specific T cells are activated using fusion proteins comprising HCV NS3, NS4, NS5a, and NS5b polypeptides, polynucleotides encoding such fusion proteins, or polypeptide or polynucleotide compositions containing the individual components of these fusions. The method can be used in model systems to develop HCV-specific immunogenic compositions, as well as to immunize a mammal against HCV.
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公开(公告)号:US07285539B2
公开(公告)日:2007-10-23
申请号:US10357619
申请日:2003-02-03
申请人: Xavier Paliard , Michael Houghton , Mark Selby
发明人: Xavier Paliard , Michael Houghton , Mark Selby
CPC分类号: C07K14/005 , A61K48/00 , A61K2039/53 , C07K2319/00 , C12N2770/24222
摘要: The invention provides a method of activating hepatitis C virus (HCV)-specific T cells, including CD4+ and CD8+ T cells. HCV-specific T cells are activated using fusion proteins comprising HCV NS3, NS4, NS5a, and NS5b polypeptides, polynucleotides encoding such fusion proteins, or polypeptide or polynucleotide compositions containing the individual components of these fusions. The method can be used in model systems to develop HCV-specific immunogenic compositions, as well as to immunize a mammal against HCV.
摘要翻译: 本发明提供一种激活丙型肝炎病毒(HCV)特异性T细胞,包括CD4 +和CD8 + T细胞的方法。 使用包含HCV NS3,NS4,NS5a和NS5b多肽的融合蛋白,编码这种融合蛋白的多核苷酸或含有这些融合物的各个组分的多肽或多核苷酸组合物来激活HCV特异性T细胞。 该方法可以在模型系统中用于开发HCV特异性免疫原性组合物,以及免疫哺乳动物抗HCV。
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公开(公告)号:US07439058B2
公开(公告)日:2008-10-21
申请号:US10715665
申请日:2003-11-17
申请人: Mark Selby , Edward Glazer , Michael Houghton
发明人: Mark Selby , Edward Glazer , Michael Houghton
CPC分类号: C07K14/005 , A61K2039/5258 , A61K2039/53 , C07K2319/00 , C12N2730/10122 , C12N2770/24322
摘要: Chimeric antigens derived from hepatitis B virus (HBV) and hepatitis C virus (HCV) are described which form virus-like particles when co-expressed with an excess of hepatitis B virus surface antigen (HBsAg). The chimeric antigens are fusion proteins containing an immunogenic peptide derived from an HCV protein coupled to the amino terminus of HBsAg. Also described are nucleic acid constructs and vectors for transfection of cells and expression of the chimeric antigens. The invention further provides methods for producing HBV/HCV virus-like particles containing the chimeric antigens, cell lines for producing the virus-like particles, combination vaccines containing the virus-like particles, and DNA vaccines that express the virus-like particles.
摘要翻译: 描述了源自乙型肝炎病毒(HBV)和丙型肝炎病毒(HCV)的嵌合抗原,当与过量的乙型肝炎病毒表面抗原(HBsAg)共表达时,形成病毒样颗粒。 嵌合抗原是含有衍生自与HBsAg的氨基末端偶联的HCV蛋白的免疫原性肽的融合蛋白。 还描述了用于转染细胞和嵌合抗原表达的核酸构建体和载体。 本发明还提供了生产含有嵌合抗原的HBV / HCV病毒样颗粒的方法,用于产生病毒样颗粒的细胞系,含病毒样颗粒的组合疫苗和表达病毒样颗粒的DNA疫苗。
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公开(公告)号:US07449566B2
公开(公告)日:2008-11-11
申请号:US11195009
申请日:2005-08-02
CPC分类号: C07K14/005 , A61K39/00 , A61K47/593 , A61K47/62 , A61K2039/53 , A61K2039/57 , C12N2770/24222
摘要: Polypeptides comprising a mutant non-structural Hepatitis C virus useful in diagnostic and/or immunogenic compositions are disclosed, in which the mutant is an N-terminal mutation that functionally disrupts the catalytic domain of NS3. Polynucleotides encoding these polypeptides, host cells transformed with polynucleotides and methods of using the polypeptides and polynucleotides are also disclosed.
摘要翻译: 公开了包含可用于诊断和/或免疫原性组合物的突变非结构性丙型肝炎病毒的多肽,其中所述突变体是功能性破坏NS3的催化结构域的N-末端突变。 还公开了编码这些多肽的多核苷酸,用多核苷酸转化的宿主细胞和使用多肽和多核苷酸的方法。
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公开(公告)号:US20110159039A1
公开(公告)日:2011-06-30
申请号:US12871035
申请日:2010-08-30
CPC分类号: C07K14/005 , A61K9/167 , A61K31/7088 , A61K39/12 , A61K39/29 , A61K2039/53 , A61K2039/55511 , A61K2039/55555 , A61K2039/55566 , A61K2039/57 , C12N2770/24222 , C12N2770/24234
摘要: Described herein is a method of eliciting antibodies and neutralizing of binding antibodies against a hepatitis C virus (HCV) E1E2 or E2 antigen using HCV E2 or HCV E1E2 polypeptides and/or HCV E2 or E1E2 polynucleotides. Elicitation of anti-E2 antibodies and anti-E2 NOB antibodies can be used, inter alia, to provide model systems to optimize anti-E2 antibody responses and/or anti-E2 NOB antibody responses to HCV and to provide prophylactic or therapeutic treatment against HCV infection.
摘要翻译: 本文描述的是使用HCV E2或HCV E1E2多肽和/或HCV E2或E1E2多核苷酸引发抗体并中和针对丙型肝炎病毒(HCV)E1E2或E2抗原的结合抗体的方法。 可以使用抗E2抗体和抗E2 NOB抗体的引发,以提供模型系统来优化抗E2抗体应答和/或抗HCV NOB抗体对HCV的反应,并提供针对HCV的预防或治疗性治疗 感染。
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公开(公告)号:US07888004B2
公开(公告)日:2011-02-15
申请号:US12287006
申请日:2008-10-03
CPC分类号: C07K14/005 , A61K39/00 , A61K47/593 , A61K47/62 , A61K2039/53 , A61K2039/57 , C12N2770/24222
摘要: Polypeptides comprising a mutant non-structural Hepatitis C virus useful in diagnostic and/or immunogenic compositions are disclosed, in which the mutant is an N-terminal mutation that functionally disrupts the catalytic domain of NS3. Polynucleotides encoding these polypeptides, host cells transformed with polynucleotides and methods of using the polypeptides and polynucleotides are also disclosed.
摘要翻译: 公开了包含可用于诊断和/或免疫原性组合物的突变非结构性丙型肝炎病毒的多肽,其中所述突变体是功能性破坏NS3的催化结构域的N-末端突变。 还公开了编码这些多肽的多核苷酸,用多核苷酸转化的宿主细胞和使用多肽和多核苷酸的方法。
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公开(公告)号:US20080095800A1
公开(公告)日:2008-04-24
申请号:US12001920
申请日:2007-12-13
CPC分类号: C07K14/005 , A61K9/167 , A61K31/7088 , A61K39/12 , A61K39/29 , A61K2039/53 , A61K2039/55511 , A61K2039/55555 , A61K2039/55566 , A61K2039/57 , C12N2770/24222 , C12N2770/24234
摘要: Described herein is a method of eliciting antibodies and neutralizing of binding antibodies against a hepatitis C virus (HCV) E1E2 or E2 antigen using HCV E2 or HCV E1E2 polypeptides and/or HCV E2 or E1E2 polynucleotides. Elicitation of anti-E2 antibodies and anti-E2 NOB antibodies can be used, inter alia, to provide model systems to optimize anti-E2 antibody responses and/or anti-E2 NOB antibody responses to HCV and to provide prophylactic or therapeutic treatment against HCV infection.
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10.发明授权Hepatitis C E1 and E2 truncated polypeptides and methods of obtaining the same 有权丙型肝炎E1和E2截短的多肽及其获得方法公开(公告)号:US06326171B1
公开(公告)日:2001-12-04
申请号:US09415582
申请日:1999-10-08
申请人: Mark Selby , Michael Houghton
发明人: Mark Selby , Michael Houghton
IPC分类号: C12N1509
CPC分类号: C07K14/005 , A61K39/00 , C12N2770/24222 , Y10S530/826
摘要: Novel Hepatitis C E1 and E2 truncated polypeptides and complexes comprising these polypeptides, are disclosed. The polypeptides are C-terminally truncated to remove all or a portion of their membrane spanning domains. Hence, the polypeptides are capable of secretion when expressed recombinantly.
摘要翻译: 公开了新型丙型肝炎E1和E2截短的多肽和包含这些多肽的复合物。 多肽被C-末端截短以除去其跨膜结构域的全部或部分。 因此,当重组表达时,多肽能够分泌。
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