公开(公告)号：US07569683B2

公开(公告)日：2009-08-04

申请号：US12044818

申请日：2008-03-07

申请人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

发明人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

IPC分类号： C07H21/04

CPC分类号： C07K14/212 ,  A61K39/00 ,  C07K16/1217

摘要： The present invention discloses the existence of two novel proteins UspA1 and UspA2, and their respective genes uspA1 and uspA2. Each protein encompasses a region that is conserved between the two proteins and comprises an epitope that is recognized by the MAb 17C7. One or more than one of these species may aggregate to form the very high molecular weight form (i.e. greater than 200 kDa) of the UspA antigen. Compositions and both diagnostic and therapeutic methods for the treatment and study of M. catarrhalis are disclosed.

摘要翻译： 本发明公开了两种新型蛋白质UspA1和UspA2及其各自的基因uspA1和uspA2的存在。 每个蛋白质包含在两种蛋白质之间保守的区域，并且包含由MAb 17C7识别的表位。 这些物质中的一种或多于一种可能聚集形成UspA抗原的非常高分子量形式（即大于200kDa）。 公开了组合物以及用于治疗和研究卡他莫拉菌的诊断和治疗方法。

公开(公告)号：US06753417B2

公开(公告)日：2004-06-22

申请号：US09952267

申请日：2001-09-12

申请人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

发明人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

IPC分类号： C07H2104

CPC分类号： C07K14/212 ,  A61K39/00 ,  C07K16/1217

摘要： The present invention discloses the existence of two novel proteins UspA1 and UspA2, and their respective genes uspA1 and uspA2. Each protein encompasses a region that is conserved between the two proteins and comprises an epitope that is recognized by the MAb 17C7. One or more than one of these species may aggregate to form the very high molecular weight form (i.e. greater than 200 kDa) of the UspA antigen. Compositions and both diagnostic and therapeutic methods for the treatment and study of M. catarrhalis are disclosed.

摘要翻译： 本发明公开了两种新型蛋白质UspA1和UspA2及其各自的基因uspA1和uspA2的存在。 每个蛋白质包含在两种蛋白质之间保守的区域，并且包含由MAb 17C7识别的表位。 这些物质中的一种或多于一种可能聚集形成UspA抗原的非常高分子量形式（即大于200kDa）。 公开了组合物以及用于治疗和研究卡他莫拉菌的诊断和治疗方法。

公开(公告)号：US06310190B1

公开(公告)日：2001-10-30

申请号：US09336447

申请日：1999-06-21

申请人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

发明人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

IPC分类号： C07H2104

CPC分类号： C07K14/212 ,  A61K39/00 ,  C07K16/1217

摘要： The present invention discloses the existence of two novel proteins UspA1 and UspA2, and their respective genes uspA1 and uspA2. Each protein encompasses a region that is conserved between the two proteins and comprises an epitope that is recognized by the MAb 17C7. One or more than one of these species may aggregate to form the very high molecular weight form (i.e. greater than 200 kDa) of the UspA antigen. Compositions and both diagnostic and therapeutic methods for the treatment and study of M. catarrhalis are disclosed.

摘要翻译： 本发明公开了两种新型蛋白质UspA1和UspA2及其各自的基因uspA1和uspA2的存在。 每个蛋白质包含在两种蛋白质之间保守的区域，并且包含由MAb 17C7识别的表位。 这些物质中的一种或多于一种可能聚集形成UspA抗原的非常高分子量形式（即大于200kDa）。 公开了组合物以及用于治疗和研究卡他莫拉菌的诊断和治疗方法。

公开(公告)号：US07344724B2

公开(公告)日：2008-03-18

申请号：US10872769

申请日：2004-06-21

申请人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

发明人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

IPC分类号： A61K39/02

CPC分类号： C07K14/212 ,  A61K39/00 ,  C07K16/1217

摘要： The present invention discloses the existence of two novel proteins UspA1 and UspA2, and their respective genes uspA1 and uspA2. Each protein encompasses a region that is conserved between the two proteins and comprises an epitope that is recognized by the MAb 17C7. One or more than one of these species may aggregate to form the very high molecular weight form (i.e. greater than 200 kDa) of the UspA antigen. Compositions and both diagnostic and therapeutic methods for the treatment and study of M. catarrhalis are disclosed.

摘要翻译： 本发明公开了两种新型蛋白质UspA1和UspA2及其各自的基因uspA1和uspA2的存在。 每个蛋白质包含在两种蛋白质之间保守的区域，并且包含由MAb 17C7识别的表位。 这些物质中的一种或多于一种可以聚集形成UspA抗原的非常高分子量形式（即大于200kDa）。 公开了组合物以及用于治疗和研究卡他莫拉菌的诊断和治疗方法。

公开(公告)号：US07288646B2

公开(公告)日：2007-10-30

申请号：US10872768

申请日：2004-06-21

申请人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

发明人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

IPC分类号： C07H21/04

CPC分类号： C07K14/212 ,  A61K39/00 ,  C07K16/1217

摘要： The present invention discloses the existence of two novel proteins UspA1 and UspA2, and their respective genes uspA1 and uspA2. Each protein encompasses a region that is conserved between the two proteins and comprises an epitope that is recognized by the MAb 17C7. One or more than one of these species may aggregate to form the very high molecular weight form (ie. greater than 200 kDa) of the UspA antigen. Compositions and both diagnostic and therapeutic methods for the treatment and study of M catarrhalis are disclosed.

摘要翻译： 本发明公开了两种新型蛋白质UspA1和UspA2及其各自的基因uspA1和uspA2的存在。 每个蛋白质包含在两种蛋白质之间保守的区域，并且包含由MAb 17C7识别的表位。 这些物质中的一种或多于一种可能聚集形成UspA抗原的非常高分子量形式（即大于200kDa）。 公开了治疗和研究卡他莫拉胶囊的组合物和诊断和治疗方法。

公开(公告)号：US07576194B2

公开(公告)日：2009-08-18

申请号：US12044805

申请日：2008-03-07

申请人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

发明人： Eric J. Hansen ,  Christoph Aebi ,  Leslie D. Cope ,  Isobel Maciver ,  Michael J. Fiske ,  Ross A. Fredenburg

IPC分类号： C07H21/04

CPC分类号： C07K14/212 ,  A61K39/00 ,  C07K16/1217

摘要： The present invention discloses the existence of two novel proteins UspA1 and UspA2, and their respective genes uspA1 and uspA2. Each protein encompasses a region that is conserved between the two proteins and comprises an epitope that is recognized by the MAb 17C7. One or more than one of these species may aggregate to form the very high molecular weight form (i.e. greater than 200 kDa) of the UspA antigen. Compositions and both diagnostic and therapeutic methods for the treatment and study of M. catarrhalis are disclosed.

摘要翻译： 本发明公开了两种新型蛋白质UspA1和UspA2及其各自的基因uspA1和uspA2的存在。 每个蛋白质包含在两种蛋白质之间保守的区域，并且包含由MAb 17C7识别的表位。 这些物质中的一种或多于一种可能聚集形成UspA抗原的非常高分子量形式（即大于200kDa）。 公开了组合物以及用于治疗和研究卡他莫拉菌的诊断和治疗方法。

公开(公告)号：US5993826A

公开(公告)日：1999-11-30

申请号：US25363

申请日：1993-03-02

申请人： Eric J. Hansen ,  Meria E. Helminen ,  Isobel Maciver

发明人： Eric J. Hansen ,  Meria E. Helminen ,  Isobel Maciver

IPC分类号： A61K38/00 ,  A61K39/00 ,  A61P31/04 ,  C07K14/21 ,  C07K16/12 ,  C12P21/08 ,  A61K39/102 ,  A61K39/02 ,  C07K14/285 ,  C07K16/102

CPC分类号： C07K16/1203 ,  C07K14/212 ,  C07K16/1214 ,  C07K16/1217 ,  A61K2039/505 ,  A61K38/00 ,  A61K39/00

摘要： The present disclosure relates to Moraxella catarrhalis outer membrane vesicle (OMV) compositions, to selected antigenic proteins from the outer membranes of M. catarrhalis which have a variety of useful properties, and to monoclonal antibodies against these proteins. Particular "Outer Membrane Proteins" (OMPs) of the invention are characterized as having molecular weights of about 30 kD, 80 kD (also termed CopB protein) and between about 200 and 700 kD (HMWP antigen). Passive immunization with monoclonal antibodies directed against these proteins confers protection against homologous and heterologous Moraxella catarrhalis strains in animal models, and active immunization with outer membrane vesicles also enhances pulmonary clearance of distinct M. catarrhalis strains. This demonstrates both the utility of antibodies in conferring passive immunity and the usefulness of OMPs, or variants thereof, in the preparation of vaccines. Also disclosed are DNA segments encoding these OMPs, methods for preparing the antigens, or variants, through the application of recombinant DNA techniques, as well as diagnostic methods and related embodiments.

公开(公告)号：US5599693A

公开(公告)日：1997-02-04

申请号：US450002

申请日：1995-05-25

申请人： Eric J. Hansen ,  Merja Helminen ,  Isobel Maciver

发明人： Eric J. Hansen ,  Merja Helminen ,  Isobel Maciver

IPC分类号： A61K39/095 ,  A61K38/00 ,  A61K39/00 ,  A61K39/02 ,  A61K39/395 ,  A61P31/04 ,  C07K14/195 ,  C07K14/21 ,  C07K16/00 ,  C07K16/12 ,  C12N1/21 ,  C12N15/00 ,  C12N15/02 ,  C12N15/09 ,  C12N15/31 ,  C12P21/00 ,  C12P21/08 ,  C12R1/01 ,  C12R1/19 ,  C12R1/91 ,  G01N33/53 ,  G01N33/569 ,  G01N33/577 ,  C12P21/06

CPC分类号： C07K16/1203 ,  C07K14/212 ,  C07K16/1217 ,  A61K38/00 ,  A61K39/00

摘要： The present disclosure relates to selected antigenic proteins obtained from the outer membranes of Moraxella catarrhalis, that have been found by the inventors to have a variety of useful properties. These proteins, termed OMPs ("Outer Membrane Proteins"), are characterized as having molecular weights of 30, 80 and 100 kD, respectively. Studies set forth herein demonstrate that monoclonal antibodies directed against these proteins confer a protective effect against infection by Moraxella catarrhalis organisms in animal models, demonstrating the potential usefulness of such antibodies in conferring passive immunity as well as the potential usefulness of these OMPs, or variants thereof, in the preparation of vaccines. Also disclosed are DNA segments encoding these OMPs, methods for preparing the antigens, or variants, through the application of recombinant DNA techniques, as well as diagnostic methods and embodiments.

摘要翻译： 本公开涉及从本发明人已经发现的具有各种有用特性的从卡他莫拉菌的外膜获得的选定抗原蛋白。 称为OMP（“外膜蛋白”）的这些蛋白质的特征分别为分子量分别为30,80和100kD。 本文所述的研究表明，针对这些蛋白质的单克隆抗体对动物模型中的莫拉菌素卡他莫斯生物的感染具有保护作用，证明了这种抗体在赋予被动免疫力方面的潜在用途以及这些OMP或其变体的潜在用途 ，在疫苗的制备中。 还公开了编码这些OMP的DNA片段，通过应用重组DNA技术制备抗原或变体的方法，以及诊断方法和实施方案。

公开(公告)号：US5552146A

公开(公告)日：1996-09-03

申请号：US745591

申请日：1991-08-15

申请人： Eric J. Hansen ,  Merja Helminen ,  Isobel Maciver

发明人： Eric J. Hansen ,  Merja Helminen ,  Isobel Maciver

IPC分类号： A61K39/095 ,  A61K38/00 ,  A61K39/00 ,  A61K39/02 ,  A61K39/395 ,  A61P31/04 ,  C07K14/195 ,  C07K14/21 ,  C07K16/00 ,  C07K16/12 ,  C12N1/21 ,  C12N15/00 ,  C12N15/02 ,  C12N15/09 ,  C12N15/31 ,  C12P21/00 ,  C12P21/08 ,  C12R1/01 ,  C12R1/19 ,  C12R1/91 ,  G01N33/53 ,  G01N33/569 ,  G01N33/577 ,  A61K39/95 ,  A61K39/40 ,  C07K14/22

CPC分类号： C07K16/1203 ,  C07K14/212 ,  C07K16/1217 ,  A61K38/00 ,  A61K39/00

摘要： The present disclosure relates to selected antigenic proteins obtained from the outer membranes of Moraxella catarrhalis, that have been found by the inventors to have a variety of useful properties. These proteins, termed OMPs ("Outer Membrane Proteins"), are characterized as having molecular weights of 30, 80 and 100 kD, respectively. Studies set forth herein demonstrate that monoclonal antibodies directed against these proteins confer a protective effect against infection by Moraxella catarrhalis organisms in animal models, demonstrating the potential usefulness of such antibodies in conferring passive immunity as well as the potential usefulness of these OMPs, or variants thereof, in the preparation of vaccines. Also disclosed are DNA segments encoding these OMPs, methods for preparing the antigens, or variants, through the application of recombinant DNA techniques, as well as diagnostic methods and embodiments.

摘要翻译： 本公开涉及从本发明人已经发现的具有各种有用特性的从卡他莫拉菌的外膜获得的选定抗原蛋白。 称为OMP（“外膜蛋白”）的这些蛋白质的特征分别为分子量分别为30,80和100kD。 本文所述的研究表明，针对这些蛋白质的单克隆抗体对动物模型中的莫拉菌素卡他莫斯生物的感染具有保护作用，证明了这种抗体在赋予被动免疫力方面的潜在用途以及这些OMP或其变体的潜在用途 ，在疫苗的制备中。 还公开了编码这些OMP的DNA片段，通过应用重组DNA技术制备抗原或变体的方法，以及诊断方法和实施方案。

公开(公告)号：US5981213A

公开(公告)日：1999-11-09

申请号：US450351

申请日：1995-05-25

申请人： Eric J. Hansen ,  Merja E. Helminen ,  Isobel Maciver

发明人： Eric J. Hansen ,  Merja E. Helminen ,  Isobel Maciver

IPC分类号： A61K38/00 ,  A61K39/00 ,  A61P31/04 ,  C07K14/21 ,  C07K16/12 ,  C12P21/08 ,  C12P21/06 ,  C07H21/02 ,  C12N1/12 ,  C12N15/00

CPC分类号： C07K16/1203 ,  C07K14/212 ,  C07K16/1214 ,  C07K16/1217 ,  A61K2039/505 ,  A61K38/00 ,  A61K39/00

摘要： The present disclosure relates to Moraxella catarrhalis outer membrane vesicle (OMV) compositions, to selected antigenic proteins from the outer membranes of M. catarrhalis which have a variety of useful properties, and to monoclonal antibodies against these proteins. Particular "Outer Membrane Proteins" (OMPs) of the invention are characterized as having molecular weights of about 30 kD, 80 kD (also termed CopB protein) and between about 200 and 700 kD (HMWP antigen). Passive immunization with monoclonal antibodies directed against these proteins confers protection against homologous and heterologous Moraxella catarrhalis strains in animal models, and active immunization with outer membrane vesicles also enhances pulmonary clearance of distinct M. catarrhalis strains. This demonstrates both the utility of antibodies in conferring passive immunity and the usefulness of OMPs, or variants thereof, in the preparation of vaccines. Also disclosed are DNA segments encoding these OMPs, methods for preparing the antigens, or variants, through the application of recombinant DNA techniques, as well as diagnostic methods and related embodiments.

摘要翻译： 本公开内容涉及卡他莫拉菌外膜囊泡（OMV）组合物，具有多种有用特性的卡他莫拉胶囊的外膜的选定抗原蛋白质以及针对这些蛋白质的单克隆抗体。 本发明的特定的“外膜蛋白”（OMP）的特征在于具有约30kD，80kD（也称为CopB蛋白）和约200至700kD（HMWP抗原）的分子量。 用针对这些蛋白质的单克隆抗体的被动免疫赋予动物模型中的同源和异源卡他莫拉菌株的保护，并且与外膜囊泡的主动免疫也增强了不同的卡他莫拉菌株的肺清除。 这证明了抗体在赋予被动免疫中的效用以及OMP或其变体在制备疫苗中的用途。 还公开了编码这些OMP的DNA片段，通过应用重组DNA技术制备抗原或变体的方法，以及诊断方法和相关实施方案。