公开(公告)号：US20110182948A1

公开(公告)日：2011-07-28

申请号：US12993393

申请日：2009-05-22

申请人： Beka Solomon ,  Oded Grinstein ,  Nir Friedman ,  Michal Arbel ,  Haim Tsubery ,  Richar Fisher

发明人： Beka Solomon ,  Oded Grinstein ,  Nir Friedman ,  Michal Arbel ,  Haim Tsubery ,  Richar Fisher

IPC分类号： A61K9/00 ,  A61K38/02 ,  A61K35/76 ,  A61P25/00 ,  A61P25/28 ,  A61P25/16 ,  B82Y5/00

CPC分类号： A61K35/76 ,  A61K35/74 ,  A61K49/1896 ,  C12N2770/00011 ,  C12N2770/00042 ,  C12N2795/14111 ,  C12N2795/14142 ,  Y02A50/473

摘要： The present invention relates to the use of a filamentous agent other than a filamentous bacteriophage to disaggregate aggregated proteins in plaque or to treat a patient suffering from or susceptible to a disease characterized by the presence of plaque.

摘要翻译： 本发明涉及除了丝状噬菌体以外的丝状药物在斑块中分解聚集的蛋白质或用于治疗患有特征为斑块特征的疾病或易感的患者的用途。

公开(公告)号：US20100041867A1

公开(公告)日：2010-02-18

申请号：US12540169

申请日：2009-08-12

申请人： Yoram SHECHTER ,  Matityahu Fridkin ,  Haim Tsubery

发明人： Yoram SHECHTER ,  Matityahu Fridkin ,  Haim Tsubery

IPC分类号： A61K47/48 ,  C07D207/40 ,  C07D403/02 ,  C07K2/00 ,  C07D403/12

CPC分类号： A61K47/60 ,  A61K31/7036 ,  A61K38/1709 ,  A61K38/212 ,  A61K38/22 ,  A61K38/2242 ,  A61K38/2278 ,  A61K38/26 ,  A61K38/27 ,  A61K38/28 ,  A61K47/54 ,  A61K47/545 ,  C07D207/404 ,  C07D207/416 ,  C07D207/452 ,  C07D403/12

摘要： Reversible pegylated drugs are provided by derivatization of free functional groups of the drug selected from amino, hydroxyl, mercapto, phosphate and/or carboxyl with groups sensitive to mild basic conditions such as 9-fluorenylmethoxycarbonyl (Fmoc) or 2-sulfo-9-fluorenylmethoxycarbonyl (FMS), to which group a PEG moiety is attached. In these pegylated drugs, the PEG moiety and the drug residue are not linked directly to each other, but rather both residues are linked to different positions of the scaffold Fmoc or FMS structure that is highly sensitive to bases and is removable under physiological conditions. The drugs are preferably drugs containing an amino group, most preferably peptides and proteins of low or medium molecular weight. Similar molecules are provided wherein a protein carrier or another polymer carrier replaces the PEG moiety.

摘要翻译： 可逆的聚乙二醇化药物通过衍生自选自氨基，羟基，巯基，磷酸酯和/或羧基的药物的游离官能团与对温和碱性条件敏感的基团如9-芴基甲氧基羰基（Fmoc）或2-磺基-9-芴基甲氧基羰基 （FMS），连接有PEG部分的基团。 在这些聚乙二醇化药物中，PEG部分和药物残留物不直接相互连接，而是两个残基都连接到对碱基高度敏感并在生理条件下可去除的支架Fmoc或FMS结构的不同位置。 药物优选是含有氨基的药物，最优选低分子量或中等分子量的肽和蛋白质。 提供了类似的分子，其中蛋白质载体或另一种聚合物载体取代了PEG部分。

公开(公告)号：US08343910B2

公开(公告)日：2013-01-01

申请号：US12540169

申请日：2009-08-12

申请人： Yoram Shechter ,  Matityahu Fridkin ,  Haim Tsubery

发明人： Yoram Shechter ,  Matityahu Fridkin ,  Haim Tsubery

IPC分类号： A61K38/00

CPC分类号： A61K47/60 ,  A61K31/7036 ,  A61K38/1709 ,  A61K38/212 ,  A61K38/22 ,  A61K38/2242 ,  A61K38/2278 ,  A61K38/26 ,  A61K38/27 ,  A61K38/28 ,  A61K47/54 ,  A61K47/545 ,  C07D207/404 ,  C07D207/416 ,  C07D207/452 ,  C07D403/12

摘要： Reversible pegylated drugs are provided by derivatization of free functional groups of the drug selected from amino, hydroxyl, mercapto, phosphate and/or carboxyl with groups sensitive to mild basic conditions such as 9-fluorenylmethoxycarbonyl (Fmoc) or 2-sulfo-9-fluorenylmethoxycarbonyl (FMS), to which group a PEG moiety is attached. In these pegylated drugs, the PEG moiety and the drug residue are not linked directly to each other, but rather both residues are linked to different positions of the scaffold Fmoc or FMS structure that is highly sensitive to bases and is removable under physiological conditions. The drugs are preferably drugs containing an amino group, most preferably peptides and proteins of low or medium molecular weight. Similar molecules are provided wherein a protein carrier or another polymer carrier replaces the PEG moiety.

公开(公告)号：US07585837B2

公开(公告)日：2009-09-08

申请号：US11244402

申请日：2005-10-06

申请人： Yoram Shechter ,  Matityahu Fridkin ,  Haim Tsubery

发明人： Yoram Shechter ,  Matityahu Fridkin ,  Haim Tsubery

IPC分类号： A61K38/00 ,  A61K47/48 ,  C07K2/00

CPC分类号： A61K47/60 ,  A61K31/7036 ,  A61K38/1709 ,  A61K38/212 ,  A61K38/22 ,  A61K38/2242 ,  A61K38/2278 ,  A61K38/26 ,  A61K38/27 ,  A61K38/28 ,  A61K47/54 ,  A61K47/545 ,  C07D207/404 ,  C07D207/416 ,  C07D207/452 ,  C07D403/12

摘要： Reversible pegylated drugs are provided by derivatization of free functional groups of the drug selected from amino, hydroxyl, mercapto, phosphate and/or carboxyl with groups sensitive to mild basic conditions such as 9-fluorenylmethoxycarbonyl (Fmoc) or 2-sulfo-9-fluorenylmethoxycarbonyl (FMS), to which group a PEG moiety is attached. In these pegylated drugs, the PEG moiety and the drug residue are not linked directly to each other, but rather both residues are linked to different positions of the scaffold Fmoc or FMS structure that is highly sensitive to bases and is removable under physiological conditions. The drugs are preferably drugs containing an amino group, most preferably peptides and proteins of low or medium molecular weight. Similar molecules are provided wherein a protein carrier or another polymer carrier replaces the PEG moiety.

摘要翻译： 可逆的聚乙二醇化药物通过衍生自选自氨基，羟基，巯基，磷酸酯和/或羧基的药物的游离官能团与对温和碱性条件敏感的基团如9-芴基甲氧基羰基（Fmoc）或2-磺基-9-芴基甲氧基羰基 （FMS），连接有PEG部分的基团。 在这些聚乙二醇化药物中，PEG部分和药物残留物不直接相互连接，而是两个残基都连接到对碱基高度敏感并在生理条件下可去除的支架Fmoc或FMS结构的不同位置。 药物优选是含有氨基的药物，最优选低分子量或中等分子量的肽和蛋白质。 提供了类似的分子，其中蛋白质载体或另一种聚合物载体取代了PEG部分。

公开(公告)号：US07435716B2

公开(公告)日：2008-10-14

申请号：US10451795

申请日：2002-01-16

申请人： Itzhak Ofek ,  Matityahu Fridkin ,  Haim Tsubery

发明人： Itzhak Ofek ,  Matityahu Fridkin ,  Haim Tsubery

IPC分类号： A61K38/02 ,  A61K38/08 ,  A61K38/10 ,  A61K38/12 ,  C07K2/00 ,  C07K7/00

CPC分类号： C07K7/62 ,  A61K38/00 ,  C07K5/1016

摘要： Novel conjugates of bacterial outer membrane binding peptides, preferably having bacterial sensitization activity, and immune cells chemotactic peptides, and pharmaceutical compositions containing same useful in the treatment of bacteremia and/or septicemia following infection by gram negative bacteria administered alone or in combination with conventional antibiotics.

摘要翻译： 细菌外膜结合肽的新结合物，优选具有细菌致敏活性，和免疫细胞趋化肽，以及含有可用于单独施用或与常规抗生素组合的革兰氏阴性细菌感染后的菌血症和/或败血症的药物组合物 。

公开(公告)号：US20130116175A1

公开(公告)日：2013-05-09

申请号：US13731989

申请日：2012-12-31

申请人： Yoram SHECHTER ,  Matityahu Fridkin ,  Haim Tsubery

发明人： Yoram SHECHTER ,  Matityahu Fridkin ,  Haim Tsubery

IPC分类号： A61K38/28 ,  A61K38/26

CPC分类号： A61K47/60 ,  A61K31/7036 ,  A61K38/1709 ,  A61K38/212 ,  A61K38/22 ,  A61K38/2242 ,  A61K38/2278 ,  A61K38/26 ,  A61K38/27 ,  A61K38/28 ,  A61K47/54 ,  A61K47/545 ,  C07D207/404 ,  C07D207/416 ,  C07D207/452 ,  C07D403/12

摘要： Reversible pegylated drugs are provided by derivatization of free functional groups of the drug selected from amino, hydroxyl, mercapto, phosphate and/or carboxyl with groups sensitive to mild basic conditions such as 9-fluorenylmethoxycarbonyl (Fmoc) or 2-sulfo-9-fluorenylmethoxycarbonyl (FMS), to which group a PEG moiety is attached. In these pegylated drugs, the PEG moiety and the drug residue are not linked directly to each other, but rather both residues are linked to different positions of the scaffold Fmoc or FMS structure that is highly sensitive to bases and is removable under physiological conditions. The drugs are preferably drugs containing an amino group, most preferably peptides and proteins of low or medium molecular weight. Similar molecules are provided wherein a protein carrier or another polymer carrier replaces the PEG moiety.

公开(公告)号：US20060171920A1

公开(公告)日：2006-08-03

申请号：US11244402

申请日：2005-10-06

申请人： Yoram Shechter ,  Matityahu Fridkin ,  Haim Tsubery

发明人： Yoram Shechter ,  Matityahu Fridkin ,  Haim Tsubery

IPC分类号： A61K38/28 ,  A61K38/22 ,  A61K38/21 ,  A61K38/19 ,  C07K14/575 ,  C07K14/535 ,  C07K14/56

CPC分类号： A61K47/60 ,  A61K31/7036 ,  A61K38/1709 ,  A61K38/212 ,  A61K38/22 ,  A61K38/2242 ,  A61K38/2278 ,  A61K38/26 ,  A61K38/27 ,  A61K38/28 ,  A61K47/54 ,  A61K47/545 ,  C07D207/404 ,  C07D207/416 ,  C07D207/452 ,  C07D403/12

摘要： Reversible pegylated drugs are provided by derivatization of free functional groups of the drug selected from amino, hydroxyl, mercapto, phosphate and/or carboxyl with groups sensitive to mild basic conditions such as 9-fluorenylmethoxycarbonyl (Fmoc) or 2-sulfo-9-fluorenylmethoxycarbonyl (FMS), to which group a PEG moiety is attached. In these pegylated drugs, the PEG moiety and the drug residue are not linked directly to each other, but rather both residues are linked to different positions of the scaffold Fmoc or FMS structure that is highly sensitive to bases and is removable under physiological conditions. The drugs are preferably drugs containing an amino group, most preferably peptides and proteins of low or medium molecular weight. Similar molecules are provided wherein a protein carrier or another polymer carrier replaces the PEG moiety.