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公开(公告)号:US07378092B2
公开(公告)日:2008-05-27
申请号:US11129359
申请日:2005-05-16
申请人: Irun R. Cohen , Varda Rotter , Roland Wolkowicz , Pedro Ruiz , Neta Erez-Alon , Johannes Herkel
发明人: Irun R. Cohen , Varda Rotter , Roland Wolkowicz , Pedro Ruiz , Neta Erez-Alon , Johannes Herkel
IPC分类号: A61K39/395 , A61K39/00
CPC分类号: C07K16/30 , A61K39/00 , A61K2039/505 , A61K2039/51 , C07K16/18 , C07K2317/565 , C07K2317/73
摘要: The invention relates to methods of inducing an anti-tumor immunity and/or inducing an immune responses to p53 in mammals. The methods comprise administering to a mammal an effective amount of at least one immunogen selected from the group consisting of: (i) a peptide based on a CDR of the heavy or light chain of an anti-p53 mAb, which peptide is capable of eliciting antibodies to p53; and (ii) a DNA molecule coding for the variable (V) region of an anti-p53 mAb in a suitable gene delivery vehicle. Preferably the immunogen is administered in the form of a pharmaceutical composition. Preferably the peptide is 7 to 30 amino acid residues in length and contains a sequence of the CDR2 or CDR3 of the heavy chain, or of the CDR3 of the light chain of an anti-p53 mAb.
摘要翻译: 本发明涉及在哺乳动物中诱导抗肿瘤免疫和/或诱导对p53的免疫应答的方法。 所述方法包括向哺乳动物施用有效量的选自以下的至少一种免疫原:(i)基于抗p53mAb的重链或轻链的CDR的肽,所述肽能够引发 p53抗体; 和(ii)在合适的基因递送载体中编码抗p53mAb的可变(V)区的DNA分子。 优选地,免疫原以药物组合物的形式施用。 优选地,肽的长度为7至30个氨基酸残基,并且含有重链的CDR2或CDR3的序列,或抗-p53mAb的轻链的CDR3的序列。
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公开(公告)号:US07118744B2
公开(公告)日:2006-10-10
申请号:US10032482
申请日:2002-01-02
申请人: Irun R Cohen , Varda Rotter , Roland Wolkowicz , Pedro Ruiz , Neta Erez-Alon , Johannes Herkel
发明人: Irun R Cohen , Varda Rotter , Roland Wolkowicz , Pedro Ruiz , Neta Erez-Alon , Johannes Herkel
IPC分类号: A61K39/395 , C07P16/00 , C12P21/08
CPC分类号: C07K16/30 , A61K39/00 , A61K2039/505 , A61K2039/51 , C07K16/18 , C07K2317/565 , C07K2317/73
摘要: The invention relates to the use of an immunogen selected from the group consisting of (i) an anti-p53 mAb; (ii) a fragment of an anti-p53 mAb; (iii) a peptide based on a CDR of the heavy or light chain of an anti-p53 mAb, which peptide is capable of eliciting antibodies to p53; and (iv) a DNA molecule coding for the variable (V) region of an anti-p53 mAb in a suitable gene delivery vehicle, for the preparation of a pharmaceutical composition useful for induction of anti-tumor immunity in mammals, for activating an enhanced immune response to a p53 molecule in mammals, and/or for induction of immune responses to mutated and wild-type forms of a p53 in mammals. The use of anti-p53 mAbs and novel peptides based on the CDR2 and CDR3 of the heavy chains and CDR3 of the light chains of different anti-p53 mAbs are disclosed.
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公开(公告)号:US20090098116A1
公开(公告)日:2009-04-16
申请号:US11943255
申请日:2007-11-20
申请人: Irun R. Cohen , Varda Rotter , Roland Wolkowicz , Pedro Ruiz , Neta Erez-Alon , Johannes Herkel
发明人: Irun R. Cohen , Varda Rotter , Roland Wolkowicz , Pedro Ruiz , Neta Erez-Alon , Johannes Herkel
IPC分类号: A61K39/395 , A61K31/711
CPC分类号: C07K16/30 , A61K39/00 , A61K2039/505 , A61K2039/51 , C07K16/18 , C07K2317/565 , C07K2317/73
摘要: The invention relates to the use of an immunogen selected from the group consisting of(i) an anti-p53 mAb;(ii) a fragment of an anti-p53 mAb;(iii) a peptide based on a CDR of the heavy or light chain of an anti-p53 mAb, which peptide is capable of eliciting antibodies to p53; and(iv) a DNA molecule coding for the variable (V) region of an anti-p53 mAb in a suitable gene delivery vehicle,for the preparation of a pharmaceutical composition useful for induction of anti-tumor immunity in mammals, for activating an enhanced immune response to a p53 molecule in mammals, and/or for induction of immune responses to mutated and wild-type forms of a p53 in mammals. The use of anti-p53 mAbs and novel peptides based on the CDR2 and CDR3 of the heavy chains and CDR3 of the light chains of different anti-p53 mAbs are disclosed.
摘要翻译: 本发明涉及选自以下的免疫原的用途:(i)抗p53 mAb; (ii)抗p53 mAb的片段; (iii)基于抗p53 mAb的重链或轻链的CDR的肽,该肽能够引发针对p53的抗体; 和(iv)编码合适的基因递送载体中抗p53mAb的可变(V)区的DNA分子,用于制备用于诱导哺乳动物抗肿瘤免疫的药物组合物,用于激活增强的 对哺乳动物中p53分子的免疫应答,和/或用于诱导哺乳动物中突变和野生型形式的p53的免疫应答。 公开了使用抗p53 mAb和基于不同抗p53 mAb的轻链的CDR2和CDR3的CDR3和新型肽。
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公开(公告)号:US20050208065A1
公开(公告)日:2005-09-22
申请号:US11129359
申请日:2005-05-16
申请人: Irun Cohen , Varda Rotter , Roland Wolkowicz , Pedro Ruiz , Neta Erez-Alon , Johannes Herkel
发明人: Irun Cohen , Varda Rotter , Roland Wolkowicz , Pedro Ruiz , Neta Erez-Alon , Johannes Herkel
CPC分类号: C07K16/30 , A61K39/00 , A61K2039/505 , A61K2039/51 , C07K16/18 , C07K2317/565 , C07K2317/73
摘要: The invention relates to methods of inducing an anti-tumor immunity and/or inducing an immune responses to p53 in mammals. The methods comprise administering to a mammal an effective amount of at least one immunogen selected from the group consisting of: (i) a peptide based on a CDR of the heavy or light chain of an anti-p53 mAb, which peptide is capable of eliciting antibodies to p53; and (ii) a DNA molecule coding for the variable (V) region of an anti-p53 mAb in a suitable gene delivery vehicle. Preferably the immunogen is administered in the form of a pharmaceutical composition. Preferably the peptide is 7 to 30 amino acid residues in length and contains a sequence of the CDR2 or CDR3 of the heavy chain, or of the CDR3 of the light chain of an anti-p53 mAb.
摘要翻译: 本发明涉及在哺乳动物中诱导抗肿瘤免疫和/或诱导对p53的免疫应答的方法。 所述方法包括向哺乳动物施用有效量的选自以下的至少一种免疫原:(i)基于抗p53mAb的重链或轻链的CDR的肽,所述肽能够引发 p53抗体; 和(ii)在合适的基因递送载体中编码抗p53mAb的可变(V)区的DNA分子。 优选地,免疫原以药物组合物的形式施用。 优选地,肽的长度为7至30个氨基酸残基并且包含重链的CDR2或CDR3的序列或抗p53mAb的轻链的CDR3的序列。
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公开(公告)号:US08067008B2
公开(公告)日:2011-11-29
申请号:US11573707
申请日:2005-08-23
申请人: Johannes Herkel , Irun R. Cohen , Varda Rotter , Ansgar W. Lohse , Neta Erez , Avishai Mimran , Na'aman Kam
发明人: Johannes Herkel , Irun R. Cohen , Varda Rotter , Ansgar W. Lohse , Neta Erez , Avishai Mimran , Na'aman Kam
CPC分类号: A61K39/0008 , A61K38/00 , A61K39/0005 , C07K7/06 , C07K7/08 , C07K14/435
摘要: The present invention relates to peptides capable of inhibiting cellular and immune stress responses in a eukaryotic cell. The invention provides compositions and methods for the treatment of human degenerative diseases and inflammation, utilizing these peptides.
摘要翻译: 本发明涉及能够抑制真核细胞中的细胞和免疫应答反应的肽。 本发明提供了利用这些肽治疗人退行性疾病和炎症的组合物和方法。
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公开(公告)号:US08790653B2
公开(公告)日:2014-07-29
申请号:US13287098
申请日:2011-11-01
申请人: Johannes Herkel , Irun R. Cohen , Varda Rotter , Ansgar W. Lohse , Neta Erez , Avishai Mimran , Na'aman Kam
发明人: Johannes Herkel , Irun R. Cohen , Varda Rotter , Ansgar W. Lohse , Neta Erez , Avishai Mimran , Na'aman Kam
IPC分类号: A61K39/00 , A61K38/00 , A61K38/08 , A61K38/10 , A61K38/16 , C07K16/18 , C07K7/00 , C07K7/06 , C07K7/08 , C07K14/00
CPC分类号: A61K39/0008 , A61K38/00 , A61K39/0005 , C07K7/06 , C07K7/08 , C07K14/435
摘要: The present invention relates to peptides capable of inhibiting cellular and immune stress responses in a eukaryotic cell. The invention provides compositions and methods for the treatment of human degenerative diseases and inflammation, utilizing these peptides.
摘要翻译: 本发明涉及能够抑制真核细胞中的细胞和免疫应答反应的肽。 本发明提供了利用这些肽治疗人退行性疾病和炎症的组合物和方法。
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公开(公告)号:US20120171233A1
公开(公告)日:2012-07-05
申请号:US13287098
申请日:2011-11-01
申请人: Johannes Herkel , Irun R. Cohen , Varda Rotter , Ansgar W. Lohse , Neta Erez , Avishai Mimran , Na'aman Kam
发明人: Johannes Herkel , Irun R. Cohen , Varda Rotter , Ansgar W. Lohse , Neta Erez , Avishai Mimran , Na'aman Kam
IPC分类号: A61K39/00 , A61P25/08 , A61P17/00 , A61P29/00 , A61P19/00 , A61P5/16 , A61P7/06 , A61P21/04 , A61P25/28 , A61P25/16 , A61P27/06 , A61P27/02 , A61P3/10 , A61P19/04 , A61P37/06 , A61P19/02 , A61P1/00 , A61P11/00 , A61P17/06 , A61P9/10 , A61P1/16 , A61P13/12 , A61P15/08 , A61P25/00
CPC分类号: A61K39/0008 , A61K38/00 , A61K39/0005 , C07K7/06 , C07K7/08 , C07K14/435
摘要: The present invention relates to peptides capable of inhibiting cellular and immune stress responses in a eukaryotic cell. The invention provides compositions and methods for the treatment of human degenerative diseases and inflammation, utilizing these peptides.
摘要翻译: 本发明涉及能够抑制真核细胞中的细胞和免疫应答反应的肽。 本发明提供了利用这些肽治疗人退行性疾病和炎症的组合物和方法。
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公开(公告)号:US20080267983A1
公开(公告)日:2008-10-30
申请号:US11573707
申请日:2005-08-23
申请人: Johannes Herkel , Irun R. Cohen , Varda Rotter , Ansgar W. Lohse , Neta Erez , Avishai Mimran , Na'aman Kam
发明人: Johannes Herkel , Irun R. Cohen , Varda Rotter , Ansgar W. Lohse , Neta Erez , Avishai Mimran , Na'aman Kam
CPC分类号: A61K39/0008 , A61K38/00 , A61K39/0005 , C07K7/06 , C07K7/08 , C07K14/435
摘要: The present invention relates to peptides capable of inhibiting cellular and immune stress responses in a eukaryotic cell. The invention provides compositions and methods for the treatment of human degenerative diseases and inflammation, utilizing peptides recognized by monoclonal anti-DNA antibodies, the peptides having anti-apoptotic and anti-inflammatory activity. The invention further provides antibody molecules and uses thereof for the isolation of such peptides.
摘要翻译: 本发明涉及能够抑制真核细胞中的细胞和免疫应答反应的肽。 本发明提供了使用由单克隆抗DNA抗体识别的肽,具有抗凋亡和抗炎活性的肽来治疗人退行性疾病和炎症的组合物和方法。 本发明还提供抗体分子及其用于分离这些肽的用途。
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9.发明授权Compositions of HSP60 peptides and viral antigens for vaccination and diagnosis 失效HSP60肽和病毒抗原的组合物用于疫苗接种和诊断公开(公告)号:US08652439B2
公开(公告)日:2014-02-18
申请号:US13164411
申请日:2011-06-20
CPC分类号: A61K47/4833 , A61K47/646 , A61K2039/6043 , A61K2039/64 , C07K14/005 , C12N2770/24122 , G01N33/56983 , Y02A50/386 , Y02A50/388 , Y02A50/39 , Y02A50/394 , Y02A50/53 , Y02A50/60
摘要: The present invention provides improved vaccines comprising an isolated viral antigenic peptide and a synthetic peptide derived from a T cell epitope of HSP60. The invention includes mixtures where the peptide serves as an adjuvant as well as conjugates where the peptide is covalently linked to the viral antigen. The known synthetic peptide carrier, p458, provides significantly improved immunogenicity for synthetic viral epitopes and analogs. Ec27 is a novel peptide derived from HSP60 which increases the immunogenicity substantially of the viral antigen both as a mixture or a covalent conjugate. Some of the isolated viral epitopes are novel and are claimed for diagnostic as well as therapeutic or prophylactic uses.
摘要翻译: 本发明提供了包含分离的病毒抗原肽和衍生自HSP60的T细胞表位的合成肽的改进的疫苗。 本发明包括其中肽用作佐剂以及其中肽与病毒抗原共价连接的缀合物的混合物。 已知的合成肽载体p458为合成的病毒表位和类似物提供显着改善的免疫原性。 Ec27是从HSP60衍生的新型肽,其作为混合物或共价缀合物增加了病毒抗原的免疫原性。 一些分离的病毒表位是新的,并且被要求用于诊断以及治疗或预防用途。
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10.发明申请Treatment of systemic lupus erythematosus by down-regulating the autoimmune response to autoantigens 审中-公开通过下调对自身抗原的自身免疫反应来治疗系统性红斑狼疮公开(公告)号:US20060030524A1
公开(公告)日:2006-02-09
申请号:US11179820
申请日:2005-07-13
申请人: Irun Cohen , Varda Rotter , Neta Erez , Johannes Herkel
发明人: Irun Cohen , Varda Rotter , Neta Erez , Johannes Herkel
CPC分类号: C07K14/4746 , A61K38/00 , A61K39/00 , A61K2039/505 , C07K16/18 , C07K16/4241 , G01N33/564 , G01N2800/104
摘要: Systemic lupus erythematosus (SLE) can be prevented or treated by down-regulating the autoimmune response to the C-terminal-DNA-binding domain of the p53 protein (p53) by an active principle selected from the group consisting of: (i) a peptide of, or comprising, the C-terminal DNA-binding domain of the p53 protein; (ii) a monoclonal antibody (mAb) specific for said domain of p53 (Ab1), and fragments thereof; (iii) an mAb specific for Ab1 (hereinafter Ab2), and fragments thereof; (iv) a peptide based on a complementarity determining region (CDR) of the heavy or light chain of said Ab1 or Ab2; (v) a DNA molecule coding for (i) and (iv) of for the variable region of said Ab1 and Ab2 of (ii) and (iii); and (vi) T cells specific for (i) to (iv), fragments thereof, T cell receptor (TCR) thereof and peptides comprising the variable region of said TCR. SLE can also be diagnosed by assaying for antibodies (Ab1) against the C-terminal DNA-binding domain of p53 or antibodies (Ab2) specific to the Ab1 antibodies.
摘要翻译: 可以通过选自以下的活性成分下调对自身免疫应答p53蛋白(p53)的C末端-DNA结合结构域的自身免疫应答来防止或治疗系统性红斑狼疮(SLE):(i) 或包含p53蛋白的C-末端DNA结合结构域的肽; (ii)对所述p53结构域(Ab1)特异的单克隆抗体(mAb)及其片段; (iii)Ab1(以下称Ab2)特异性的mAb及其片段; (iv)基于所述Ab1或Ab2的重链或轻链的互补决定区(CDR)的肽; (v)编码(i)和(iv)的(ii)和(iii)所述Ab1和Ab2的可变区的DNA分子; 和(vi)特异于(i)至(iv)的T细胞,其片段,T细胞受体(TCR)和包含所述TCR的可变区的肽。 也可以通过测定针对p53的C末端DNA结合结构域的抗体(Ab1)或Ab1抗体特异性抗体(Ab2)来诊断SLE。
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