公开(公告)号：US20100099145A1

公开(公告)日：2010-04-22

申请号：US12555742

申请日：2009-09-08

申请人： Haitao WANG ,  Chungsheng Mao ,  Jizhi Li ,  Jing XU ,  Rui ZHANG ,  Ling Wang ,  Yong Du ,  Longbin LIU

发明人： Haitao WANG ,  Chungsheng Mao ,  Jizhi Li ,  Jing XU ,  Rui ZHANG ,  Ling Wang ,  Yong Du ,  Longbin LIU

IPC分类号： C12P21/00 ,  C07H21/04 ,  C12N5/16

CPC分类号： C07K14/505 ,  A61K9/0019 ,  A61K38/00 ,  A61K47/6811 ,  C07K2317/53 ,  C07K2319/30

摘要： A recombinant fusion protein comprising a human erythropoietin peptide portion linked to an immunoglobulin peptide portion is described. The fusion protein has a prolonged half-life in vivo in comparison to naturally occurring or recombinant native human erythropoietin. In one embodiment of the invention, the protein has a half-life in vivo at least three fold higher than native human erythropoietin. The fusion protein also exhibits enhanced erythropoietic bioactivity in comparison to native human erythropoietin. In one embodiment, the fusion protein comprises the complete peptide sequence of a human erythropoietin (EPO) molecule and the peptide sequence of an Fc fragment of human immunoglobulin IgG1. The Fc fragment in the fusion protein includes the hinge region, CH2 and CH3 domains of human immunoglobulin IgG1. The EPO molecule may be linked directly to the Fc fragment to avoid extraneous peptide linkers and lessen the risk of an immunogenic response when administered in vivo. In one embodiment the hinge region is a human Fc fragment variant having a non-cysteine residue at amino acid 6. The invention also relates to nucleic acid and amino acid sequences encoding the fusion protein and transfected cell lines and methods for producing the fusion protein. The invention further includes pharmaceutical compositions comprising the fusion protein and methods of using the fusion protein and/or the pharmaceutical compositions, for example to stimulate erythropoiesis in subjects in need of therapy.

公开(公告)号：US20100099612A1

公开(公告)日：2010-04-22

申请号：US12555759

申请日：2009-09-08

申请人： Haitao WANG ,  Chungsheng MAO ,  Jizhi LI ,  Jing XU ,  Rui ZHANG ,  Ling WANG ,  Yong DU ,  Longbin LIU

发明人： Haitao WANG ,  Chungsheng MAO ,  Jizhi LI ,  Jing XU ,  Rui ZHANG ,  Ling WANG ,  Yong DU ,  Longbin LIU

IPC分类号： A61K38/16 ,  A61P35/00 ,  A61P31/12

CPC分类号： C07K14/56 ,  A61K38/00 ,  C07K14/555

摘要： This application relates to recombinant human interferon-like proteins. In one embodiment a recombinant protein created by gene shuffling technology is described having enhanced anti-viral and anti-proliferative activities in comparison to naturally occurring human interferon alpha 2b (HuIFN-α2b). The invention encompasses a polynucleotide encoding the protein and recombinant vectors and host cells comprising the polynucleotide. Preferably the polynucleotide is selected from the group of polynucleotides each having a sequence at least 93% identical to SEQ ID: No. 1 and the protein is selected from the group of proteins each having an amino acid sequence at least 85% identical to SEQ ID No: 2. The proteins and compositions comprising the proteins can be used for treatment of conditions responsive to interferon therapy, such as viral diseases and cancer.

摘要翻译： 本申请涉及重组人类干扰素样蛋白。 在一个实施方案中，与天然存在的人类干扰素α2b（HuIFN-α2b）相比，描述了通过基因改组技术产生的重组蛋白质具有增强的抗病毒和抗增殖活性。 本发明包括编码蛋白质的多核苷酸和包含多核苷酸的重组载体和宿主细胞。 优选地，多核苷酸选自各自具有与SEQ ID：No.1至少93％相同的序列的多核苷酸，并且所述蛋白质选自蛋白质组，其各自具有与SEQ ID NO：至少85％相同的氨基酸序列 否：2.包含蛋白质的蛋白质和组合物可用于治疗对干扰素治疗（例如病毒性疾病和癌症）有反应的病症。

公开(公告)号：US20100098716A1

公开(公告)日：2010-04-22

申请号：US12555743

申请日：2009-09-08

申请人： Haitao WANG ,  Chungsheng Mao ,  Jizhi Li ,  Jing XU ,  Rui ZHANG ,  Ling Wang ,  DU Yong ,  Longbin LIU

发明人： Haitao WANG ,  Chungsheng Mao ,  Jizhi Li ,  Jing XU ,  Rui ZHANG ,  Ling Wang ,  DU Yong ,  Longbin LIU

IPC分类号： A61K39/395 ,  A61K38/00

CPC分类号： C07K14/505 ,  A61K9/0019 ,  A61K38/00 ,  A61K47/6811 ,  C07K2317/53 ,  C07K2319/30

摘要： A recombinant fusion protein comprising a human erythropoietin peptide portion linked to an immunoglobulin peptide portion is described. The fusion protein has a prolonged half-life in vivo in comparison to naturally occurring or recombinant native human erythropoietin. In one embodiment of the invention, the protein has a half-life in vivo at least three fold higher than native human erythropoietin. The fusion protein also exhibits enhanced erythropoietic bioactivity in comparison to native human erythropoietin. In one embodiment, the fusion protein comprises the complete peptide sequence of a human erythropoietin (EPO) molecule and the peptide sequence of an Fc fragment of human immunoglobulin IgG1. The Fc fragment in the fusion protein includes the hinge region, CH2 and CH3 domains of human immunoglobulin IgG1. The EPO molecule may be linked directly to the Fc fragment to avoid extraneous peptide linkers and lessen the risk of an immunogenic response when administered in vivo. In one embodiment the hinge region is a human Fc fragment variant having a non-cysteine residue at amino acid 6. The invention also relates to nucleic acid and amino acid sequences encoding the fusion protein and transfected cell lines and methods for producing the fusion protein. The invention further includes pharmaceutical compositions comprising the fusion protein and methods of using the fusion protein and/or the pharmaceutical compositions, for example to stimulate erythropoiesis in subjects in need of therapy.

摘要翻译： 描述了包含与免疫球蛋白肽部分连接的人促红细胞生成素肽部分的重组融合蛋白。 与天然存在的或重组的天然人促红细胞生成素相比，融合蛋白在体内具有延长的半衰期。 在本发明的一个实施方案中，蛋白质的体内半衰期比天然人促红细胞生成素高至少三倍。 与天然人促红细胞生成素相比，融合蛋白也表现出增强的红细胞生物活性。 在一个实施方案中，融合蛋白包含人促红细胞生成素（EPO）分子的完整肽序列和人免疫球蛋白IgG1的Fc片段的肽序列。 融合蛋白中的Fc片段包括人免疫球蛋白IgG1的铰链区，CH2和CH3结构域。 EPO分子可以直接连接到Fc片段，以避免外来的肽接头并且当在体内施用时减轻免疫原性应答的风险。 在一个实施方案中，铰链区是在氨基酸6具有非半胱氨酸残基的人Fc片段变体。本发明还涉及编码融合蛋白和转染细胞系的核酸和氨基酸序列以及用于产生融合蛋白的方法。 本发明还包括包含融合蛋白的药物组合物和使用融合蛋白和/或药物组合物的方法，例如刺激需要治疗的受试者的红细胞生成。

公开(公告)号：US20130189226A1

公开(公告)日：2013-07-25

申请号：US13841679

申请日：2013-03-15

申请人： Haitao WANG ,  Chunsheng MAO ,  Jizhi LI ,  Ling WANG ,  Yong DU ,  Longbin LIU ,  Jing XU ,  Rui ZHANG

发明人： Haitao WANG ,  Chunsheng MAO ,  Jizhi LI ,  Ling WANG ,  Yong DU ,  Longbin LIU ,  Jing XU ,  Rui ZHANG

IPC分类号： C07K14/56

CPC分类号： C07K14/56 ,  A61K38/00 ,  C07K14/555

摘要： This application relates to recombinant human interferon-like proteins. In one embodiment a recombinant protein created by gene shuffling technology is described having enhanced anti-viral and anti-proliferative activities in comparison to naturally occurring human inteferon like alpha 2b (HuIFN-α2b). The invention encompasses a polynucleotide encoding the protein and recombinant vectors and host cells comprising the polynucleotide. Preferably the polynucleotide is selected from the group of polynucleotides each having a sequence at least 93% identical to SEQ ID: No. 1 and the protein is selected from the group of proteins each having an amino acid sequence at least 85% identical to SEQ ID No: 2. The proteins and compositions comprising the proteins can be used for treatment of conditions responsive to interferon therapy, such as viral diseases and cancer.

摘要翻译： 本申请涉及重组人类干扰素样蛋白。 在一个实施方案中，描述了与天然存在的人类干扰素如α2b（HuIFN-α2b）相比，通过基因改组技术产生的重组蛋白具有增强的抗病毒和抗增殖活性。 本发明包括编码蛋白质的多核苷酸和包含多核苷酸的重组载体和宿主细胞。 优选地，多核苷酸选自各自具有与SEQ ID：No.1至少93％相同的序列的多核苷酸，并且所述蛋白质选自蛋白质组，其各自具有与SEQ ID NO：至少85％相同的氨基酸序列 否：2.包含蛋白质的蛋白质和组合物可用于治疗对干扰素治疗（例如病毒性疾病和癌症）有反应的病症。

公开(公告)号：US20100129904A1

公开(公告)日：2010-05-27

申请号：US12555762

申请日：2009-09-08

申请人： Haitao WANG ,  Chunsheng MAO ,  Jizhi LI ,  Jing XU ,  Rui ZHANG ,  Ling WANG ,  Yong DU ,  Longbin LIU

发明人： Haitao WANG ,  Chunsheng MAO ,  Jizhi LI ,  Jing XU ,  Rui ZHANG ,  Ling WANG ,  Yong DU ,  Longbin LIU

IPC分类号： C12N5/10 ,  C07H21/04 ,  C12N15/63 ,  C12N1/21

CPC分类号： C07K14/56 ,  A61K38/00 ,  C07K14/555

摘要： This application relates to recombinant human interferon-like proteins. In one embodiment a recombinant protein created by gene shuffling technology is described having enhanced anti-viral and anti-proliferative activities in comparison to naturally occurring human interferon alpha 2b (HuIFN-α2b). The invention encompasses a polynucleotide encoding the protein and recombinant vectors and host cells comprising the polynucleotide. Preferably the polynucleotide is selected from the group of polynucleotides each having a sequence at least 93% identical to SEQ ID: No. 1 and the protein is selected from the group of proteins each having an amino acid sequence at least 85% identical to SEQ ID No: 2. The proteins and compositions comprising the proteins can be used for treatment of conditions responsive to interferon therapy, such as viral diseases and cancer.

公开(公告)号：US20090081218A1

公开(公告)日：2009-03-26

申请号：US12180455

申请日：2008-07-25

申请人： Haitao WANG ,  Yong DU ,  Rui ZHANG ,  Jing XU ,  Longbin LIU

发明人： Haitao WANG ,  Yong DU ,  Rui ZHANG ,  Jing XU ,  Longbin LIU

IPC分类号： A61K39/395 ,  C07K16/18 ,  C12N9/50 ,  C07H21/04 ,  C12P21/04 ,  C12N5/06

CPC分类号： C12N15/62 ,  A61K47/6811 ,  A61K47/6835 ,  C07K2317/53 ,  C07K2319/30

摘要： A fusion protein having a non-immunoglobulin polypeptide having a cysteine residue proximal to the C terminal thereof, and an immunoglobulin component with a mutated hinge region is provided. The mutation comprises a point mutated site corresponding in position to the position in a native hinge region of the cysteine residue located nearest the cysteine residue of the non-Ig component. The distance from the cysteine residue of the non-immunoglobulin polypeptide and any remaining cysteine residues of the mutated hinge region is sufficient to prevent the formation of a disulphide bond therebetween.

摘要翻译： 提供了具有非免疫球蛋白多肽的融合蛋白，其具有接近其C末端的半胱氨酸残基和具有突变的铰链区的免疫球蛋白组分。 该突变包括位于位于最接近非Ig组分的半胱氨酸残基的半胱氨酸残基的天然铰链区的位置的点突变位点。 与非免疫球蛋白多肽的半胱氨酸残基和突变的铰链区的任何剩余半胱氨酸残基的距离足以防止其间形成二硫键。

公开(公告)号：US20130224198A1

公开(公告)日：2013-08-29

申请号：US13872790

申请日：2013-04-29

申请人： Haitao WANG ,  Yong DU ,  Rui ZHANG ,  Jing XU ,  Longbin LIU

发明人： Haitao WANG ,  Yong DU ,  Rui ZHANG ,  Jing XU ,  Longbin LIU

IPC分类号： A61K47/48 ,  C07K14/505

CPC分类号： C07K14/505 ,  A61K9/0019 ,  A61K38/00 ,  A61K47/6811 ,  C07K2317/53 ,  C07K2319/30

摘要： A recombinant fusion protein comprising a human erythropoietin peptide portion linked to an immunoglobulin peptide portion is described. The fusion protein has a prolonged half-life in vivo compared to naturally occurring or recombinant native human erythropoietin. In one embodiment, the protein has a half-life in vivo at least three-fold higher than native human erythropoietin. The fusion protein exhibits enhanced erythropoietic bioactivity compared to native human erythropoietin. In one embodiment, the fusion protein comprises the complete peptide sequence of a human erythropoietin (EPO) molecule and the peptide sequence of an Fc fragment of human IgG1, which Fc fragment includes the hinge region, CH2 and CH3 domains. The EPO molecule may be linked directly to the Fc fragment to avoid extraneous peptide linkers and lessen risk of an immunogenic response when administered. In one embodiment the hinge region is a human Fc fragment variant having a non-cysteine residue at amino acid 6.

摘要翻译： 描述了包含与免疫球蛋白肽部分连接的人促红细胞生成素肽部分的重组融合蛋白。 与天然存在的或重组的天然人促红细胞生成素相比，融合蛋白具有延长的体内半衰期。 在一个实施方案中，蛋白质的体内半衰期比天然人促红细胞生成素高至少三倍。 与天然人促红细胞生成素相比，融合蛋白表现出增强的红细胞生物活性。 在一个实施方案中，融合蛋白包含人促红细胞生成素（EPO）分子的完整肽序列和人IgG1的Fc片段的肽序列，所述Fc片段包括铰链区，CH2和CH3结构域。 EPO分子可以直接连接到Fc片段，以避免外来的肽接头，并且当施用时降低免疫原性反应的风险。 在一个实施方案中，铰链区是在氨基酸6具有非半胱氨酸残基的人Fc片段变体。

公开(公告)号：US20120100099A1

公开(公告)日：2012-04-26

申请号：US13275205

申请日：2011-10-17

申请人： Haitao WANG ,  Longbin LIU ,  Rui ZHANG ,  Jing XU ,  Yong DU

发明人： Haitao WANG ,  Longbin LIU ,  Rui ZHANG ,  Jing XU ,  Yong DU

IPC分类号： A61K38/19 ,  C12N9/48 ,  A61P43/00 ,  C12N5/10 ,  C12N15/62 ,  C07K19/00 ,  C12P21/00

CPC分类号： C12N15/62 ,  A61K47/6811 ,  A61K47/6835 ,  C07K2317/53 ,  C07K2319/30

摘要： A fusion protein having a non-immunoglobulin polypeptide having a cysteine residue proximal to the C terminal thereof, and an immunoglobulin component with a mutated hinge region is provided. The mutation comprises a point mutated site corresponding in position to the position in a native hinge region of the cysteine residue located nearest the cysteine residue of the non-Ig component. The distance from the cysteine residue of the non-immunoglobulin polypeptide and any remaining cysteine residues of the mutated hinge region is sufficient to prevent the formation of a disulphide bond therebetween.

摘要翻译： 提供了具有非免疫球蛋白多肽的融合蛋白，其具有接近其C末端的半胱氨酸残基和具有突变的铰链区的免疫球蛋白组分。 该突变包括位于位于最接近非Ig组分的半胱氨酸残基的半胱氨酸残基的天然铰链区的位置的点突变位点。 与非免疫球蛋白多肽的半胱氨酸残基和突变的铰链区的任何剩余半胱氨酸残基的距离足以防止其间形成二硫键。

公开(公告)号：US20180012078A1

公开(公告)日：2018-01-11

申请号：US15205680

申请日：2016-07-08

申请人： Reza POURNAGHI ,  Rui ZHANG

发明人： Reza POURNAGHI ,  Rui ZHANG

IPC分类号： G06K9/00 ,  G06K9/62

CPC分类号： G06K9/00771 ,  G06K9/00718 ,  G06K9/6212 ,  G06T7/246 ,  G06T7/269 ,  G06T7/292 ,  G06T7/50 ,  G06T7/77 ,  G06T2207/10016 ,  G06T2207/10024 ,  G06T2207/10028 ,  G06T2207/20072 ,  G06T2207/20076 ,  G06T2207/30196 ,  G06T2207/30232

摘要： Processes, systems, and devices for occlusion detection for video-based object tracking (VBOT) are described herein. Embodiments process video frames to compute histogram data and depth level data for the object to detect a subset of video frames for occlusion events and generate output data that identifies each video frame of the subset of video frames for the occlusion events. Threshold measurement values are used to attempt to reduce or eliminate false positives to increase processing efficiency.

公开(公告)号：US20130007755A1

公开(公告)日：2013-01-03

申请号：US13172648

申请日：2011-06-29

申请人： David D. CHAMBLISS ,  Lei LIU ,  William G. SHERMAN ,  Rui ZHANG

发明人： David D. CHAMBLISS ,  Lei LIU ,  William G. SHERMAN ,  Rui ZHANG

IPC分类号： G06F9/46

CPC分类号： G06F9/46 ,  G06F3/061 ,  G06F3/0659 ,  G06F3/067 ,  G06F9/4881 ,  G06F17/00

摘要： For managing a storage server having improving overall system performance, a first input/output (I/O) request is received. A first priority level is dynamically assigned to the first I/O request, the first I/O request associated with a performance level for an application residing on a host in communication with the storage server. A second I/O request of a second priority level is throttled to allow at least a portion of a predetermined amount of resources previously designated for performing the second I/O request to be re-allocated to performing the first I/O request. The second priority level is different than the first priority level.