公开(公告)号：US20050065207A1

公开(公告)日：2005-03-24

申请号：US10483824

申请日：2002-07-12

申请人： Michael Sommer ,  Ole Nielsen ,  Hans Petersen ,  Haleh Ahmadian ,  Henrik Pedersen ,  Peter Brosen ,  Fiona Geiser ,  James Lee ,  Geoffrey Cox ,  Olivier Dapremont ,  Christina Suteu ,  Sebastian Assenza ,  Shankar Hariharan ,  Usha Nair

发明人： Michael Sommer ,  Ole Nielsen ,  Hans Petersen ,  Haleh Ahmadian ,  Henrik Pedersen ,  Peter Brosen ,  Fiona Geiser ,  James Lee ,  Geoffrey Cox ,  Olivier Dapremont ,  Christina Suteu ,  Sebastian Assenza ,  Shankar Hariharan ,  Usha Nair

IPC分类号： A61K31/343 ,  A61P25/24 ,  C07B20060101 ,  C07C215/32 ,  C07C215/34 ,  C07D20060101 ,  C07D307/87

CPC分类号： C07C215/32 ,  C07D307/87

摘要： A novel method is provided for the manufacture of escitalopram. The method comprises chromatographic separation of the enantiomers of citalopram or an intermediate in the production of citalopram using a chiral stationary phase such as Chiralpak™ or Chiralcel™ OD. Novel chiral intermediates for the synthesis of Escitalopram made by said method are also provided.

摘要翻译： 提供了一种制备依他普仑的新方法。 该方法包括使用手性固定相（例如Chiralpak TM或Chiralcel TM OD）对西酞普兰对映异构体或西酞普兰生产中的中间体进行色谱分离。 还提供了通过所述方法制备的用于合成依他普仑的新型手性中间体。

公开(公告)号：US20110065938A1

公开(公告)日：2011-03-17

申请号：US12781048

申请日：2010-05-17

申请人： Michael B. Sommer ,  Ole Nielsen ,  Hans Petersen ,  Haleh Ahmadian ,  Henrik Pedersen ,  Peter Brosen ,  Fiona Geiser ,  James Lee ,  Geoffrey Cox ,  Olivier Dapremont ,  Christina Suteu ,  Sebastian P. Assenza ,  Shankar Hariharan ,  Usha Nair

发明人： Michael B. Sommer ,  Ole Nielsen ,  Hans Petersen ,  Haleh Ahmadian ,  Henrik Pedersen ,  Peter Brosen ,  Fiona Geiser ,  James Lee ,  Geoffrey Cox ,  Olivier Dapremont ,  Christina Suteu ,  Sebastian P. Assenza ,  Shankar Hariharan ,  Usha Nair

IPC分类号： C07D307/87 ,  C07C215/32

CPC分类号： C07C215/32 ,  C07D307/87

摘要： A novel method is provided for the manufacture of escitalopram. The method comprises chromatographic separation of the enantiomers of citalopram or an intermediate in the production of citalopram using a chiral stationary phase such as Chiralpak™ AD or Chiralcel™ OD. Novel chiral intermediates for the synthesis of Escitalopram made by said method are also provided.

摘要翻译： 提供了一种制备依他普仑的新方法。 该方法包括使用手性固定相如Chiralpak TM AD或Chiralcel TM OD，对西酞普兰对映异构体或西酞普兰生产中的中间体进行色谱分离。 还提供了通过所述方法制备的用于合成依他普仑的新型手性中间体。

公开(公告)号：US20210230381A1

公开(公告)日：2021-07-29

申请号：US17158665

申请日：2021-01-26

申请人： Mikkel Dybro Lundorf ,  Henrik Pedersen ,  NANOCORE APS

发明人： Mikkel Dybro Lundorf ,  Henrik Pedersen ,  Tore Dehli

IPC分类号： C08J5/00 ,  B82Y30/00 ,  B82Y40/00 ,  C08K9/04 ,  C08K9/08 ,  C01B32/05 ,  C01B32/174 ,  C01B32/194 ,  C04B35/565 ,  C04B35/58 ,  C04B35/50 ,  C04B35/10 ,  C04B35/56 ,  C04B35/48 ,  C04B28/02 ,  C01B32/156 ,  C01B32/168 ,  C04B14/38 ,  C04B16/06 ,  C04B35/80 ,  C08F292/00 ,  C08J5/06 ,  C09D5/24 ,  C09D11/03 ,  C09D11/04 ,  C09D11/107 ,  C09D11/52 ,  C09D133/14

摘要： A type of composite material where the matrix material and additive are held together by covalently or non-covalently bound ligands is described. A particularly useful composite material covered by the present invention is a carbon nanotube-reinforced composite material where the matrix consists of a polymer, covalently attached to a linker, where said linker is non-covalently attached to the carbon nanotube.
Methods for the preparation of such composite materials are provided.

公开(公告)号：US10336808B2

公开(公告)日：2019-07-02

申请号：US13482472

申请日：2012-05-29

申请人： Jøgen Schøller ,  Henrik Pedersen ,  Liselotte Brix

发明人： Jøgen Schøller ,  Henrik Pedersen ,  Liselotte Brix

IPC分类号： C07K14/74 ,  A61K47/64 ,  G01N33/569 ,  A61K49/18 ,  G01N33/574 ,  A61K47/61 ,  A61K38/00

摘要： Novel compounds carrying ligands capable of binding to counter receptors on relevant target cells are disclosed. The compounds possess a number of advantageous features, rendering them very suitable for a wide range of applications, including use as detection systems, detection of relevant target cells as well as a number of other methods. In particular, novel MHC complexes comprising one or more MHC molecules are disclosed. The affinity and specificity of the MHC-peptide complexes are surprisingly high. The possibility of presenting to the target cells a plurality of MHC-peptide complexes makes the MHC complexes according to the present invention an extremely powerful tool e.g. in the field of therapy and diagnosis. The invention generally relates to the field of therapy, including therapeutic methods and therapeutic compositions. Also comprised by the present invention is the sample-mounted use of MHC complexes and MHC multimers.

公开(公告)号：US20180298154A1

公开(公告)日：2018-10-18

申请号：US15525741

申请日：2015-11-11

申请人： Mikkel Dybro Lundorf ,  Henrik Pedersen ,  NANOCORE APS

发明人： Mikkel Dybro Lundorf ,  Henrik Pedersen ,  Tore Dehli

IPC分类号： C08J5/00 ,  C08F292/00 ,  C08J5/06 ,  C01B32/156 ,  C01B32/168 ,  C01B32/194 ,  C09D11/52 ,  C09D11/107 ,  C09D11/04 ,  C09D11/03 ,  C09D5/24 ,  C09D133/14 ,  C04B16/06 ,  C04B14/38 ,  C04B35/80

CPC分类号： C08J5/005 ,  B82Y30/00 ,  B82Y40/00 ,  C01B32/05 ,  C01B32/152 ,  C01B32/156 ,  C01B32/168 ,  C01B32/174 ,  C01B32/194 ,  C04B14/386 ,  C04B16/0675 ,  C04B35/80 ,  C04B2235/48 ,  C08F292/00 ,  C08F2810/20 ,  C08J5/06 ,  C08J2323/06 ,  C08J2363/00 ,  C08J2367/00 ,  C08J2369/00 ,  C08J2375/04 ,  C08J2377/06 ,  C08K3/041 ,  C08K3/042 ,  C08K9/04 ,  C08K9/08 ,  C08K2201/001 ,  C08K2201/011 ,  C09D5/24 ,  C09D11/03 ,  C09D11/04 ,  C09D11/107 ,  C09D11/52 ,  C09D133/14 ,  C22C26/00 ,  C22C2026/001 ,  H01B1/04 ,  C08L23/04

摘要： Composite material, where the matrix material and the additive are held together by covalently or non-covalently bound ligands. The linker unit between matrix and additive has the structure Ligand1-LinkerL-Ligand 2, wherein Ligand1 and Ligand2 are a bond or a chemical entity that is capable of binding covalently or non-covalently to a structural entity, such as a polymer matrix or the additive (ex. CNT, graphene, carbon nanofiber, etc), and LinkerL is a chemical bond or entity that links Ligand1 and Ligand2.

公开(公告)号：US08426183B2

公开(公告)日：2013-04-23

申请号：US13329550

申请日：2011-12-19

申请人： Bjarne Roenfeldt Nielsen ,  Allan Svendsen ,  Henrik Pedersen ,  Jesper Vind ,  Hanne Vang Hendriksen ,  Torben Peter Frandsen

发明人： Bjarne Roenfeldt Nielsen ,  Allan Svendsen ,  Henrik Pedersen ,  Jesper Vind ,  Hanne Vang Hendriksen ,  Torben Peter Frandsen

IPC分类号： C12N9/34 ,  C12P19/20 ,  C07H21/04 ,  C07K1/00

CPC分类号： C12N9/2428 ,  C12P19/14 ,  C12P19/20 ,  Y02E50/17

摘要： The invention relates to a variant of a parent fungal glucoamylase, which exhibits improved thermal stability and/or increased specific activity using saccharide substrates.

公开(公告)号：US20120264161A1

公开(公告)日：2012-10-18

申请号：US13482472

申请日：2012-05-29

申请人： Jørgen Schøller ,  Henrik Pedersen ,  Liselotte Brix

发明人： Jørgen Schøller ,  Henrik Pedersen ,  Liselotte Brix

IPC分类号： C07K19/00 ,  C12N5/0783 ,  C12Q1/02

CPC分类号： C07K14/70539 ,  A61K38/00 ,  A61K47/61 ,  A61K47/6425 ,  A61K49/1896 ,  G01N33/56905 ,  G01N33/56911 ,  G01N33/56972 ,  G01N33/56977 ,  G01N33/574 ,  G01N2333/70539 ,  G01N2800/24 ,  Y02A50/401 ,  Y02A50/55 ,  Y02A50/57 ,  Y02A50/58

摘要： Novel compounds carrying ligands capable of binding to counter receptors on relevant target cells are disclosed. The compounds possess a number of advantageous features, rendering them very suitable for a wide range of applications, including use as detection systems, detection of relevant target cells as well as a number of other methods. In particular, novel MHC complexes comprising one or more MHC molecules are disclosed. The affinity and specificity of the MHC-peptide complexes are surprisingly high. The possibility of presenting to the target cells a plurality of MHC-peptide complexes makes the MHC complexes according to the present invention an extremely powerful tool e.g. in the field of therapy and diagnosis. The invention generally relates to the field of therapy, including therapeutic methods and therapeutic compositions. Also comprised by the present invention is the sample-mounted use of MHC complexes and MHC multimers.

摘要翻译： 公开了携带能够结合相关靶细胞上的对受体的配体的新型化合物。 这些化合物具有许多有利的特征，使得它们非常适用于广泛的应用，包括用作检测系统，相关靶细胞的检测以及许多其它方法。 特别地，公开了包含一种或多种MHC分子的新型MHC复合物。 MHC-肽复合物的亲和性和特异性惊人地高。 向靶细胞呈递多个MHC-肽复合物的可能性使得根据本发明的MHC复合物成为非常强大的工具，例如， 在治疗和诊断领域。 本发明一般涉及治疗领域，包括治疗方法和治疗组合物。 本发明还包括MHC复合物和MHC多聚体的样品安装用途。

公开(公告)号：US08012732B2

公开(公告)日：2011-09-06

申请号：US12552572

申请日：2009-09-02

申请人： Janne Brunstedt ,  Jørn Dalgaard Mikkelsen ,  Henrik Pedersen ,  Jørn Borch Søe

发明人： Janne Brunstedt ,  Jørn Dalgaard Mikkelsen ,  Henrik Pedersen ,  Jørn Borch Søe

IPC分类号： C12P1/00 ,  C12N9/00 ,  C12N9/20 ,  C12N1/20 ,  C12N15/00 ,  C07H21/04

CPC分类号： A21D8/042 ,  A23C19/0328 ,  A23D7/02 ,  A23K20/189 ,  A23K50/75 ,  A23L7/107 ,  A23L7/109 ,  A23L7/111 ,  A23L27/60 ,  A23L29/06 ,  C11B3/003 ,  C12N9/18 ,  C12P7/62 ,  C12P19/44 ,  C12Y301/01

摘要： A fungal wild-type lipolytic enzyme having a higher ratio of activity on polar lipids compared with triglycerides, wherein the enzyme preferably has a phospholipid:triglyceride activity ratio of at least 4. Preferably, the lipolytic enzyme according to the present invention has a glycolipid:triglyceride hydrolyzing activity ratio of at least 1.5. In one embodiment, the fungal lipolytic enzyme according to the present invention comprises an amino acid sequence as shown in SEQ ID NO: 1 or SEQ ID No. 2 or SEQ ID No. 4 or SEQ ID No. 6 or an amino acid sequence which has at least 90% identity thereto. The present invention further encompasses a nucleic acid encoding a fungal lipolytic enzyme, which nucleic acid is selected from the group consisting of: (a) a nucleic acid comprising a nucleotide shown in SEQ ID No. 3, SEQ ID No. 5 or SEQ ID No. 7; (b) a nucleic acid which is related to the nucleotide sequence of SEQ ID No. 3, SEQ ID No. 5 or SEQ ID No. 7 by the degeneration of the genetic code; and (c) nucleic acid comprising a nucleotide sequence which has at least 90% identity with the nucleotide sequence shown in SEQ ID No. 3, SEQ ID No. 5 or SEQ ID No. 7.

摘要翻译： 与甘油三酯相比，极性脂质活性比例更高的真菌野生型脂肪分解酶，其中所述酶优选具有至少为4的磷脂：甘油三酯活性比。优选地，根据本发明的脂肪分解酶具有糖脂： 甘油三酯水解活性比至少为1.5。 在一个实施方案中，根据本发明的真菌脂肪分解酶包含如SEQ ID NO：1或SEQ ID No.2或SEQ ID No.4或SEQ ID No.6所示的氨基酸序列或氨基酸序列， 与其具有至少90％的同一性。 本发明还包括编码真菌脂肪分解酶的核酸，该核酸选自：（a）包含SEQ ID No.3，SEQ ID No.5或SEQ ID No.5所示核苷酸的核酸 第7号 （b）通过遗传密码的退化与SEQ ID No.3，SEQ ID No.5或SEQ ID No.7的核苷酸序列有关的核酸; 和（c）核酸，其包含与SEQ ID No.3，SEQ ID No.5或SEQ ID No.7所示的核苷酸序列具有至少90％同一性的核苷酸序列。

公开(公告)号：US20100248257A1

公开(公告)日：2010-09-30

申请号：US12647747

申请日：2009-12-28

申请人： Kivin Jacobsen ,  Henrik Pedersen ,  Liselotte Brix ,  Jesper Lohse ,  Jørgen Schøller ,  Tina Jakobsen

发明人： Kivin Jacobsen ,  Henrik Pedersen ,  Liselotte Brix ,  Jesper Lohse ,  Jørgen Schøller ,  Tina Jakobsen

IPC分类号： G01N33/53

CPC分类号： C07K14/70539 ,  A61K38/00 ,  A61K47/61 ,  A61K47/6425 ,  A61K47/665 ,  B82Y5/00

摘要： The present invention relates to the fields of analysis, diagnostics, prognostics, standardization, characterization and enumeration of entities such as biological cells, as well as therapeutical applications. Accordingly, the present invention in preferred aspects is directed to methods for the detection and/or analysis and/or isolation and optionally further manipulation of entities, such as cells, particles, and supra-molecular structures.

摘要翻译： 本发明涉及诸如生物细胞的实体以及治疗应用的分析，诊断，预测，标准化，表征和计数的领域。 因此，本发明在优选方面涉及用于检测和/或分析和/或分离和任选地进一步操纵诸如细胞，颗粒和超分子结构的实体的方法。

公开(公告)号：US07354753B2

公开(公告)日：2008-04-08

申请号：US10421586

申请日：2003-04-23

申请人： Bjarne Ronfeldt Nielsen ,  Allan Svendsen ,  Henrik Pedersen ,  Jesper Vind ,  Hanne Vang Hendriksen ,  Torben Peter Frandsen

发明人： Bjarne Ronfeldt Nielsen ,  Allan Svendsen ,  Henrik Pedersen ,  Jesper Vind ,  Hanne Vang Hendriksen ,  Torben Peter Frandsen

IPC分类号： C12N9/34 ,  C07H21/04

CPC分类号： C12N9/2428 ,  C12P19/20 ,  Y02E50/17

摘要： The invention relates to a variant of a parent fungal glucoamylase, which exhibits altered properties, in particular improved thermal stability and/or increased specific activity.

摘要翻译： 本发明涉及亲本真菌葡糖淀粉酶的变体，其具有改变的性质，特别是改进的热稳定性和/或增加的比活性。