公开(公告)号：US20120009207A1

公开(公告)日：2012-01-12

申请号：US13107504

申请日：2011-05-13

申请人： Li-Te CHIN ,  Shu-Ching Hsu

发明人： Li-Te CHIN ,  Shu-Ching Hsu

IPC分类号： A61K35/14 ,  A61P37/06

CPC分类号： A61K35/26 ,  A61K38/17 ,  C07K16/2818 ,  C07K2317/34 ,  C07K2317/92 ,  G01N33/505

摘要： The present invention provides a CTLA-4 non-blocking agent of a complete human antibody nature, thus is non-immunogenic in a human. The immunoassay method using such a non-blocking agent measures the CTLA-4 content in a sample of a human subject. The present invention further provides a novel method for isolating human regulatory T cells. The resultant enriched and depleted cellular populations are useful in treating or ameliorating of human diseases.

摘要翻译： 本发明提供了完全人抗体性质的CTLA-4非阻断剂，因此在人体中是非免疫原性的。 使用这种非阻断剂的免疫测定方法测量人受试者样品中的CTLA-4含量。 本发明还提供了一种分离人类调节性T细胞的新方法。 所产生的富含和消耗的细胞群可用于治疗或改善人类疾病。

公开(公告)号：US20060240006A1

公开(公告)日：2006-10-26

申请号：US11111098

申请日：2005-04-20

申请人： Chishih Chu ,  Li-Te Chin ,  Shu-Ching Hsu

发明人： Chishih Chu ,  Li-Te Chin ,  Shu-Ching Hsu

IPC分类号： G01N33/567 ,  A61K39/395 ,  C07K16/28

CPC分类号： C07K16/2818 ,  C07K2317/21

摘要： In order to provide necessary information for the production of complete human monoclonal antibodies capable of human CD152 (CTLA-4) binding, the primary structures of heavy and light chains have been elucidated. The novel amino acid sequence of identified heavy and light chains are derived from VH3 and Vλ germline genes, respectively. Antibodies comprising such novel structures cause specific binding to soluble recombinant human CD152 as well as to activated human peripheral T cells, where the expression of CD152 has been elevated.

公开(公告)号：US08021860B2

公开(公告)日：2011-09-20

申请号：US12318679

申请日：2009-01-06

申请人： Li-Te Chin ,  Shu-Ching Hsu

发明人： Li-Te Chin ,  Shu-Ching Hsu

IPC分类号： C12P21/04

CPC分类号： G01N33/5052 ,  A61K2039/505 ,  C07K16/00 ,  C07K16/2818 ,  C07K2317/73 ,  C07K2317/74 ,  G01N33/505 ,  G01N33/6854 ,  G01N2333/70521

摘要： A method for obtaining agonist, antagonist and inverse agonist, to a given physiological receptor is disclosed. For the method, use is made of in silico design synthetic immunogens, which are caused to act in vitro on human lymphocyte-containing cell populations. A preferred receptor is human CD152, particularly the regions of CDR1, CDR2 and CDR3 that elicit antibodies serving as antagonist, inverse agonist and agonist, respectively. Also provided is a method in the treatment of human peripheral lymphocytes for use in the screening of CD152 ligands that yield pharmacological effects.

摘要翻译： 公开了一种获得给定生理受体的激动剂，拮抗剂和反向激动剂的方法。 对于该方法，使用计算机设计合成免疫原，其在体外对人类含淋巴细胞的细胞群体起作用。 优选的受体是人CD152，特别是分别引发作为拮抗剂，反向激动剂和激动剂的抗体的CDR1，CDR2和CDR3的区域。 还提供了治疗人外周淋巴细胞用于筛选产生药理作用的CD152配体的方法。

公开(公告)号：US20110033895A1

公开(公告)日：2011-02-10

申请号：US12888713

申请日：2010-09-23

申请人： Li-Te CHIN ,  Shu-Ching Hsu

发明人： Li-Te CHIN ,  Shu-Ching Hsu

IPC分类号： C12P21/08

CPC分类号： G01N33/5052 ,  A61K2039/505 ,  C07K16/00 ,  C07K16/2818 ,  C07K2317/73 ,  C07K2317/74 ,  G01N33/505 ,  G01N33/6854 ,  G01N2333/70521

摘要： A method for obtaining agonist, antagonist and inverse agonist, to a given physiological receptor is disclosed. For the method, use is made of in silico design synthetic immunogens, which are caused to act in vitro on human lymphocyte-containing cell populations. A preferred receptor is human CD152, particularly the regions of CDR1, CDR2 and CDR3 that elicit antibodies serving as antagonist, inverse agonist and agonist, respectively. Also provided is a method in the treatment of human peripheral lymphocytes for use in the screening of CD152 ligands that yield pharmacological effects.

摘要翻译： 公开了一种获得给定生理受体的激动剂，拮抗剂和反向激动剂的方法。 对于该方法，使用计算机设计合成免疫原，其在体外对人类含淋巴细胞的细胞群体起作用。 优选的受体是人CD152，特别是分别引发作为拮抗剂，反向激动剂和激动剂的抗体的CDR1，CDR2和CDR3的区域。 还提供了治疗人外周淋巴细胞用于筛选产生药理作用的CD152配体的方法。

公开(公告)号：US20090286224A1

公开(公告)日：2009-11-19

申请号：US12318679

申请日：2009-01-06

申请人： Li-Te Chin ,  Shu-Ching Hsu

发明人： Li-Te Chin ,  Shu-Ching Hsu

IPC分类号： C12Q1/70 ,  G01N33/53 ,  C07K7/00 ,  C07K16/28

CPC分类号： G01N33/5052 ,  A61K2039/505 ,  C07K16/00 ,  C07K16/2818 ,  C07K2317/73 ,  C07K2317/74 ,  G01N33/505 ,  G01N33/6854 ,  G01N2333/70521

摘要： A method for obtaining agonist, antagonist and inverse agonist, to a given physiological receptor is disclosed. For the method, use is made of in silico design synthetic immunogens, which are caused to act in vitro on human lymphocyte-containing cell populations. A preferred receptor is human CD152, particularly the regions of CDR1, CDR2 and CDR3 that elicit antibodies serving as antagonist, inverse agonist and agonist, respectively. Also provided is a method in the treatment of human peripheral lymphocytes for use in the screening of CD152 ligands that yield pharmacological effects.

摘要翻译： 公开了一种获得给定生理受体的激动剂，拮抗剂和反向激动剂的方法。 对于该方法，使用计算机设计合成免疫原，其在体外对人类含淋巴细胞的细胞群体起作用。 优选的受体是人CD152，特别是分别引发作为拮抗剂，反向激动剂和激动剂的抗体的CDR1，CDR2和CDR3的区域。 还提供了治疗人外周淋巴细胞用于筛选产生药理作用的CD152配体的方法。

公开(公告)号：US10174109B2

公开(公告)日：2019-01-08

申请号：US15798478

申请日：2017-10-31

申请人： Li-Te Chin ,  Shu-Ching Hsu ,  Kai-Chen Wang

发明人： Li-Te Chin ,  Shu-Ching Hsu ,  Kai-Chen Wang

IPC分类号： C07K16/24 ,  C07K16/18 ,  A61K39/00

摘要： The present invention relates to methods of making human anti-HMGB1 antibodies, compositions comprising these antibodies and methods of using the antibodies and compositions in HMGB1 associated-neuropathy.

公开(公告)号：US09840555B2

公开(公告)日：2017-12-12

申请号：US14526842

申请日：2014-10-29

申请人： Li-Te Chin ,  Shu-Ching Hsu ,  Kai-Chen Wang

发明人： Li-Te Chin ,  Shu-Ching Hsu ,  Kai-Chen Wang

IPC分类号： C07K16/18 ,  C07K16/24 ,  A61K39/00

CPC分类号： C07K16/24 ,  A61K2039/505 ,  C07K2317/76

摘要： The present invention relates to methods of making human anti-HMGB1 antibodies, compositions comprising these antibodies and methods of using the antibodies and compositions in HMGB1 associated-neuropathy.

公开(公告)号：US07968300B2

公开(公告)日：2011-06-28

申请号：US11943682

申请日：2007-11-21

申请人： Li-Te Chin ,  Shu-Ching Hsu

发明人： Li-Te Chin ,  Shu-Ching Hsu

IPC分类号： G01N33/53

CPC分类号： A61K35/26 ,  A61K38/17 ,  C07K16/2818 ,  C07K2317/34 ,  C07K2317/92 ,  G01N33/505

摘要： The present invention provides a CTLA-4 non-blocking agent of a complete human antibody nature, thus is non-immunogenic in a human. The immunoassay method using such a non-blocking agent measures the CTLA-4 content in a sample of a human subject. The present invention further provides a novel method for isolating human regulatory T cells. The resultant enriched and depleted cellular populations are useful in treating or ameliorating of human diseases.

摘要翻译： 本发明提供了完全人抗体性质的CTLA-4非阻断剂，因此在人体中是非免疫原性的。 使用这种非阻断剂的免疫测定方法测量人受试者样品中的CTLA-4含量。 本发明还提供了一种分离人类调节性T细胞的新方法。 所产生的富含和贫化的细胞群可用于治疗或改善人类疾病。

公开(公告)号：US08158386B2

公开(公告)日：2012-04-17

申请号：US12888713

申请日：2010-09-23

申请人： Li-Te Chin ,  Shu-Ching Hsu

发明人： Li-Te Chin ,  Shu-Ching Hsu

IPC分类号： G01N33/567

CPC分类号： G01N33/5052 ,  A61K2039/505 ,  C07K16/00 ,  C07K16/2818 ,  C07K2317/73 ,  C07K2317/74 ,  G01N33/505 ,  G01N33/6854 ,  G01N2333/70521

摘要： A method for obtaining agonist, antagonist and inverse agonist, to a given physiological receptor is disclosed. For the method, use is made of in silico design synthetic immunogens, which are caused to act in vitro on human lymphocyte-containing cell populations. A preferred receptor is human CD152, particularly the regions of CDR1, CDR2 and CDR3 that elicit antibodies serving as antagonist, inverse agonist and agonist, respectively. Also provided is a method in the treatment of human peripheral lymphocytes for use in the screening of CD152 ligands that yield pharmacological effects.

摘要翻译： 公开了一种获得给定生理受体的激动剂，拮抗剂和反向激动剂的方法。 对于该方法，使用计算机设计合成免疫原，其在体外对人类含淋巴细胞的细胞群体起作用。 优选的受体是人CD152，特别是分别引发作为拮抗剂，反向激动剂和激动剂的抗体的CDR1，CDR2和CDR3的区域。 还提供了治疗人外周淋巴细胞用于筛选产生药理作用的CD152配体的方法。

公开(公告)号：US07494779B2

公开(公告)日：2009-02-24

申请号：US10866120

申请日：2004-06-14

申请人： Li-Te Chin ,  Shu-Ching Hsu

发明人： Li-Te Chin ,  Shu-Ching Hsu

IPC分类号： G01N33/53

CPC分类号： G01N33/5052 ,  A61K2039/505 ,  C07K16/00 ,  C07K16/2818 ,  C07K2317/73 ,  C07K2317/74 ,  G01N33/505 ,  G01N33/6854 ,  G01N2333/70521

摘要： A method for obtaining agonist, antagonist and inverse agonist, to a given physiological receptor is disclosed. For the method, use is made of in silico design synthetic immunogens, which are caused to act in vitro on human lymphocyte-containing cell populations. A preferred receptor is human CD152, particularly the regions of CDR1, CDR2 and CDR3 that elicit antibodies serving as antagonist, inverse agonist and agonist, respectively. Also provided is a method in the treatment of human peripheral lymphocytes for use in the screening of CD152 ligands that yield pharmacological effects.

摘要翻译： 公开了一种获得给定生理受体的激动剂，拮抗剂和反向激动剂的方法。 对于该方法，使用计算机设计合成免疫原，其在体外对人类含淋巴细胞的细胞群体起作用。 优选的受体是人CD152，特别是分别引发作为拮抗剂，反向激动剂和激动剂的抗体的CDR1，CDR2和CDR3的区域。 还提供了治疗人外周淋巴细胞用于筛选产生药理作用的CD152配体的方法。