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11.发明授权Method, computing routine, device for predicting properties of MHC/peptide complexes, and data and peptides produced therefrom 有权方法,计算程序,用于预测MHC /肽复合物的性质的装置,以及由其制备的数据和肽公开(公告)号:US07702465B2
公开(公告)日:2010-04-20
申请号:US10516628
申请日:2003-06-10
申请人: Ignace Lasters , Johan Desmet
发明人: Ignace Lasters , Johan Desmet
IPC分类号: G06F19/00 , C07K14/74 , C07K14/435
摘要: The present invention relates to a method for structure-based prediction of properties of peptides and peptide analogs in complex with major histocompatibility (MHC) class I and class II molecules. The properties mainly relate to the three-dimensional structure of an MHC/peptide complex and the binding affinity of a peptide for an MHC receptor. The invention further relates to a computer program and a device therefor. The invention further relates to data produced by a method of the invention. The invention further relates to peptides and peptide analogs predicted to bind to target-MHC molecules. The present invention thus relates to the field of immunology, with possible applications in manufacture of vaccinates, de-immunization of proteins, and manufacture of therapeutic agents, especially immunotherapeutic agents.
摘要翻译: 本发明涉及与主要组织相容性(MHC)I类和II类分子复合的肽和肽类似物的基于结构的预测性质的方法。 性质主要涉及MHC /肽复合物的三维结构和肽对MHC受体的结合亲和力。 本发明还涉及一种计算机程序及其装置。 本发明还涉及通过本发明的方法产生的数据。 本发明还涉及预期与靶MHC分子结合的肽和肽类似物。 因此,本发明涉及免疫学领域,可能应用于疫苗接种的制造,蛋白质的去免疫,以及治疗剂,特别是免疫治疗剂的制造。
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12.发明授权Method for generating information related to the molecular structure of a biomolecule 有权生成与生物分子的分子结构有关的信息的方法公开(公告)号:US08571806B2
公开(公告)日:2013-10-29
申请号:US12959224
申请日:2010-12-02
申请人: Johan Desmet , Ignace Lasters , Dominique Vlieghe , Carlo Boutton , Philippe Stas , Jan Spriet
发明人: Johan Desmet , Ignace Lasters , Dominique Vlieghe , Carlo Boutton , Philippe Stas , Jan Spriet
CPC分类号: G06F19/16 , B01J2219/00689 , B01J2219/00695 , B01J2219/007 , B01J2219/0072 , B01J2219/00722 , B01J2219/00725 , B01J2219/00731 , C07K1/00 , C07K2299/00 , C40B40/06 , C40B40/10 , C40B40/12
摘要: The present invention provides methods for generating information related to the molecular structure of a biomolecule.
摘要翻译: 本发明提供了生成与生物分子的分子结构有关的信息的方法。
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13.发明授权公开(公告)号:US08229721B1
公开(公告)日:2012-07-24
申请号:US10129513
申请日:2000-11-03
CPC分类号: G06F19/16
摘要: The invention provides methods and apparatus for analyzing a protein structure by A) receiving a reference structure (A) forming a three dimensional representation of a protein; B) substituting into the structure of (A) a pattern with amino-acids different from the one of the protein; C) optimizing the conformation of (A) substituted by pattern of (B); D) assessing the energetic compatibility (EC) of the pattern of (B) within the context of the structure of (A) being structurally optimized in (C) with respect to the pattern, by comparing the global energy of the substituted and optimized protein structure with the global energy of the non-substituted reference structure; and E) storing a value reflecting the EC of the pattern together with information related to the structure of the pattern in the form of an energetic compatibility object (ECO).
摘要翻译: 本发明提供了通过A)接收形成蛋白质的三维表示的参考结构(A)来分析蛋白质结构的方法和装置; B)用不同于蛋白质的氨基酸取代(A)结构的结构; C)优化(A)由(B)的图案取代的构象; D)通过比较取代和优化的蛋白质的全球能量,评估在(A)的结构的上下文中(B)的模式的能量相容性(EC)在(C)中相对于模式在结构上优化 具有非取代参考结构的全球能量结构; 以及E)将反映所述图案的EC的值与能量兼容对象(ECO)形式的与所述图案的结构有关的信息一起存储。
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14.发明申请公开(公告)号:US20100305304A1
公开(公告)日:2010-12-02
申请号:US12676783
申请日:2008-09-08
申请人: Johan Desmet , Ignace Lasters
发明人: Johan Desmet , Ignace Lasters
CPC分类号: C07K1/00 , C07K7/08 , C07K14/001 , C07K2318/20
摘要: The present invention is related to a non-natural, thermodynamically stable, proteinaceous scaffold consisting of three non-covalently associated peptides, wherein each peptide sequence comprises less than fifty amino acid residues and wherein at least 50% of the said residues are substitutable amino acids into at least ten different amino acid residue types. The present invention is further related to a non-natural, triple-stranded, parallel alpha-helical coiled coil scaffold wherein each of the three constituting peptide sequences comprise between 2 and 7 consecutive heptad repeats, wherein at least 50% of the core residues are isoleucines, wherein all non-core residues are alanines, and wherein the constituting peptide sequences remain associated under physical conditions that are significantly different from physiological conditions.
摘要翻译: 本发明涉及由三种非共价相关肽组成的非天然的热力学稳定的蛋白质支架,其中每个肽序列包含少于50个氨基酸的残基,并且其中至少50%的所述残基是可取代的氨基酸 至少十种不同的氨基酸残基类型。 本发明进一步涉及非天然的,三链的平行的α-螺旋卷曲的线圈支架,其中三个构成的肽序列中的每一个包含2-7个连续的七重复重复序列,其中至少50%的核心残基是 异亮氨酸,其中所有非核残基是丙氨酸,并且其中构成的肽序列在与生理条件显着不同的物理条件下保持相关。
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15.发明申请PEPTIDES FOR INDUCING A CTL AND/OR HTL RESPONSE TO HEPATITIS C VIRUS 审中-公开用于诱导针对HEPATITIS C病毒的CTL和/或HTL反应的肽公开(公告)号:US20100099613A1
公开(公告)日:2010-04-22
申请号:US12574214
申请日:2009-10-06
申请人: Marie-Ange Buyse , Geert Maertens , Erik Depla , Ignace Lasters , Johan Desmet , Denise Baker , Robert W. Chesnut , Mark Newman , Alessandra Sette , John Sidney , Scott Southwood
发明人: Marie-Ange Buyse , Geert Maertens , Erik Depla , Ignace Lasters , Johan Desmet , Denise Baker , Robert W. Chesnut , Mark Newman , Alessandra Sette , John Sidney , Scott Southwood
IPC分类号: A61K38/16 , A61K31/7052 , A61P37/00 , A61K38/10 , A61K38/08
CPC分类号: C07K14/005 , A61K39/00 , A61K39/12 , A61K39/29 , A61K2039/55566 , A61K2039/57 , C12N2770/24222 , C12N2770/24234
摘要: The present invention is directed to peptides, and nucleic acids encoding them, derived from the Hepatitis C Virus (HCV). The peptides are those which elicit a CTL and/or HTL response in a host. The invention is also directed to compositions and vaccines for prevention and treatment of HCV infection and diagnostic methods for detection of HCV exposure in patients.
摘要翻译: 本发明涉及衍生自丙型肝炎病毒(HCV)的肽和编码它们的核酸。 肽是在宿主中引起CTL和/或HTL应答的肽。 本发明还涉及用于预防和治疗HCV感染的组合物和疫苗以及用于检测患者中HCV暴露的诊断方法。
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公开(公告)号:US20080312840A1
公开(公告)日:2008-12-18
申请号:US11568108
申请日:2006-04-21
申请人: Johan Desmet , Geert Meersseman , Nathalie Boutonnet , Jurgen Pletinckx , Krista De Clercq , Ignace Lasters
发明人: Johan Desmet , Geert Meersseman , Nathalie Boutonnet , Jurgen Pletinckx , Krista De Clercq , Ignace Lasters
IPC分类号: G01N33/68
摘要: The present invention is related to a quantitative structure-based affinity scoring method for peptide/protein complexes. More specifically, the present invention comprises a method that operates on the basis of a highly specific force field function (e.g. CHARMM) that is applied to all-atom structural representations of peptide/receptor complexes. Peptide side-chain contributions to total affinity are scored after detailed rotameric sampling followed by controlled energy refinement. The method of the invention further comprises a de novo approach to estimate dehydration energies from the simulation of individual amino acids in a solvent box filled with explicit water molecules and applying the same force field function as used to evaluate peptide/receptor complex interactions.
摘要翻译: 本发明涉及肽/蛋白复合物的基于定量结构的亲和评分方法。 更具体地说,本发明包括一种基于应用于肽/受体复合物的全原子结构表示的高度特异性的力场函数(例如CHARMM)来操作的方法。 在详细的旋转异构体取样之后进行受控能量细化,对总亲和力的肽侧链贡献进行评分。 本发明的方法还包括从填充有显性水分子的溶剂盒中的各个氨基酸的模拟估算脱水能量并应用用于评估肽/受体复合物相互作用的相同的力场函数的从头方法。
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公开(公告)号:US08538706B2
公开(公告)日:2013-09-17
申请号:US13270931
申请日:2011-10-11
申请人: Johan Desmet , Geert Meersseman , Nathalie Boutonnet , Jurgen Pletinckx , Krista De Clercq , Ignace Lasters
发明人: Johan Desmet , Geert Meersseman , Nathalie Boutonnet , Jurgen Pletinckx , Krista De Clercq , Ignace Lasters
摘要: The present invention is related to a quantitative structure-based affinity scoring method for peptide/protein complexes. More specifically, the present invention comprises a method that operates on the basis of a highly specific force field function (e.g. CHARMM) that is applied to all-atom structural representations of peptide/receptor complexes. Peptide side-chain contributions to total affinity are scored after detailed rotameric sampling followed by controlled energy refinement. The method of the invention further comprises a de novo approach to estimate dehydration energies from the simulation of individual amino acids in a solvent box filled with explicit water molecules and applying the same force field function as used to evaluate peptide/receptor complex interactions.
摘要翻译: 本发明涉及肽/蛋白复合物的基于定量结构的亲和评分方法。 更具体地说,本发明包括一种基于应用于肽/受体复合物的全原子结构表示的高度特异性的力场函数(例如CHARMM)来操作的方法。 在详细的旋转异构体取样之后进行受控能量细化,对总亲和力的肽侧链贡献进行评分。 本发明的方法还包括从填充有显性水分子的溶剂盒中的各个氨基酸的模拟估算脱水能量并应用用于评估肽/受体复合物相互作用的相同的力场函数的从头方法。
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18.发明申请Method, computing routine, device for predicting properties of MHC/peptide complexes, and data and peptides produced therefrom. 审中-公开方法,计算程序,用于预测MHC /肽复合物的性质的装置,以及由其制备的数据和肽。公开(公告)号:US20100168398A1
公开(公告)日:2010-07-01
申请号:US12660774
申请日:2010-03-04
申请人: Ignace Lasters , Johan Desmet
发明人: Ignace Lasters , Johan Desmet
摘要: The present invention relates to a method for structure-based prediction of properties of peptides and peptide analogs in complex with major histocompatibility (MHC) class I and class II molecules. The said properties mainly relate to the three-dimensional structure of an MHC/peptide complex and the binding affinity of a peptide for an MHC receptor. The invention further relates to a computer program and a device therefor. The invention further relates to data produced by a method of the invention. The invention further relates to peptides and peptide analogs predicted to bind to target-MHC molecules. The present invention thus relates to the field of immunology, with possible applications in manufacture of vaccinates, de-immunization of proteins, and manufacture of therapeutic agents, especially immunotherapeutic agents.
摘要翻译: 本发明涉及与主要组织相容性(MHC)I类和II类分子复合的肽和肽类似物的基于结构的预测性质的方法。 所述性质主要涉及MHC /肽复合物的三维结构和肽对MHC受体的结合亲和力。 本发明还涉及一种计算机程序及其装置。 本发明还涉及通过本发明的方法产生的数据。 本发明还涉及预期与靶MHC分子结合的肽和肽类似物。 因此,本发明涉及免疫学领域,可能应用于疫苗接种的制造,蛋白质的去免疫,以及治疗剂,特别是免疫治疗剂的制造。
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19.发明申请Method, computing routine, device for predicting properties of mhc/peptide complexes, and data and peptides produced therefrom 有权方法,计算程序,用于预测mhc /肽复合物的性质的装置,以及由其制备的数据和肽公开(公告)号:US20060111554A1
公开(公告)日:2006-05-25
申请号:US10516628
申请日:2003-06-10
申请人: Ignace Lasters , Johan Desmet
发明人: Ignace Lasters , Johan Desmet
摘要: The present invention relates to a method for structure-based prediction of properties of peptides and peptide analogs in complex with major histocompatibility (MHC) class I and class II molecules. The said properties mainly relate to the three-dimensional structure of an MHC/peptide complex and the binding affinity of a peptide for an MHC receptor. The invention further relates to a computer program and a device therefor. The invention further relates to data produced by a method of the invention. The invention further relates to peptides and peptide analogs predicted to bind to target-MHC molecules. The present invention thus relates to the field of immunology, with possible applications in manufacture of vaccinates, de-immunization of proteins, and manufacture of therapeutic agents, especially immunotherapeutic agents.
摘要翻译: 本发明涉及与主要组织相容性(MHC)I类和II类分子复合的肽和肽类似物的基于结构的预测性质的方法。 所述性质主要涉及MHC /肽复合物的三维结构和肽对MHC受体的结合亲和力。 本发明还涉及一种计算机程序及其装置。 本发明还涉及通过本发明的方法产生的数据。 本发明还涉及预期与靶MHC分子结合的肽和肽类似物。 因此,本发明涉及免疫学领域,可能应用于疫苗接种的制造,蛋白质的去免疫,以及治疗剂,特别是免疫治疗剂的制造。
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20.发明申请公开(公告)号:US20060093617A1
公开(公告)日:2006-05-04
申请号:US11140487
申请日:2005-05-31
申请人: Marie-Ange Buyse , Geert Maertens , Erik Depla , Ignace Lasters , Johan Desmet , Denise Baker , Robert Chesnut , Mark Newman , Alessandro Sette , John Sidney , Scott Southwood
发明人: Marie-Ange Buyse , Geert Maertens , Erik Depla , Ignace Lasters , Johan Desmet , Denise Baker , Robert Chesnut , Mark Newman , Alessandro Sette , John Sidney , Scott Southwood
CPC分类号: C07K14/005 , A61K39/00 , A61K39/12 , A61K39/29 , A61K2039/55566 , A61K2039/57 , C12N2770/24222 , C12N2770/24234
摘要: The present invention is directed to peptides, and nucleic acids encoding them, derived from the Hepatitis C Virus (HCV). The peptides are those which elicit a CTL and/or HTL response in a host. The invention is also directed to compositions and vaccines for prevention and treatment of HCV infection and diagnostic methods for detection of HCV exposure in patients.
摘要翻译: 本发明涉及衍生自丙型肝炎病毒(HCV)的肽和编码它们的核酸。 肽是在宿主中引起CTL和/或HTL应答的肽。 本发明还涉及用于预防和治疗HCV感染的组合物和疫苗以及用于检测患者中HCV暴露的诊断方法。
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