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公开(公告)号:US20170159044A1
公开(公告)日:2017-06-08
申请号:US15433909
申请日:2017-02-15
Applicant: TWIST BIOSCIENCE CORPORATION
Inventor: Esteban Toro , Sebastian TREUSCH , Siyuan CHEN , Cheng-Hsien WU
CPC classification number: C12N15/1031 , C12N15/1027 , C12N15/1093 , C12N15/66 , C12P19/34
Abstract: Methods and compositions are provided for assembly of large nucleic acids where the assembled large nucleic acids lack internal sequence modifications made during the assembly process.
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公开(公告)号:US20220315971A1
公开(公告)日:2022-10-06
申请号:US17825863
申请日:2022-05-26
Applicant: Twist Bioscience Corporation
Inventor: Cheng-Hsien WU , Sebastian TREUSCH
IPC: C12P19/34
Abstract: Provided herein are methods, systems, and compositions for seamless nucleic acid assembly. Such methods, systems, and compositions for seamless nucleic acid assembly include those for in vitro recombination cloning, single-stranded hierarchal DNA assembly, or overlap extension PCR without primer removal.
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Patent Agency Ranking
公开(公告)号:US20200181667A1
公开(公告)日:2020-06-11
申请号:US16712678
申请日:2019-12-12
Applicant: TWIST BIOSCIENCE CORPORATION
Inventor: Cheng-Hsien WU , Sebastian TREUSCH
IPC: C12P19/34
Abstract: Provided herein are methods, systems, and compositions for seamless nucleic acid assembly. Such methods, systems, and compositions for seamless nucleic acid assembly include those for in vitro recombination cloning, single-stranded hierarchal DNA assembly, or overlap extension PCR without primer removal.
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公开(公告)号:US20240158955A1
公开(公告)日:2024-05-16
申请号:US18356787
申请日:2023-07-21
Applicant: TWIST BIOSCIENCE CORPORATION
Inventor: Anthony COX , Sebastian TREUSCH , Siyuan CHEN
IPC: C40B50/06 , C12N15/10 , C12N15/113 , C12Q1/6876 , C40B50/08 , C40B50/14 , G01N33/50
CPC classification number: C40B50/06 , C12N15/1079 , C12N15/1093 , C12N15/113 , C12Q1/6876 , C40B50/08 , C40B50/14 , G01N33/502 , G01N33/5029 , G01N33/5041 , C12N2320/30 , C12N2330/31 , C12Q1/6886
Abstract: Disclosed herein are methods for the generation of highly accurate oligonucleic acid libraries encoding for predetermined variants of a nucleic acid sequence. The degree of variation may be complete, resulting in a saturated variant library, or less than complete, resulting in a selective library of variants. The variant oligonucleic acid libraries described herein may designed for further processing by transcription or translation. The variant oligonucleic acid libraries described herein may be designed to generate variant RNA, DNA and/or protein populations. Further provided herein are method for identifying variant species with increased or decreased activities, with applications in regulating biological functions and the design of therapeutics for treatment or reduction of disease.
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公开(公告)号:US20220064628A1
公开(公告)日:2022-03-03
申请号:US17320127
申请日:2021-05-13
Applicant: TWIST BIOSCIENCE CORPORATION
Inventor: Esteban Toro , Sebastian TREUSCH , Siyuan CHEN , Cheng-Hsien WU
Abstract: Methods and compositions are provided for assembly of large nucleic acids where the assembled large nucleic acids lack internal sequence modifications made during the assembly process.
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公开(公告)号:US20190352635A1
公开(公告)日:2019-11-21
申请号:US16530717
申请日:2019-08-02
Applicant: TWIST BIOSCIENCE CORPORATION
Inventor: Esteban Toro , Sebastian TREUSCH , Siyuan CHEN , Cheng-Hsien WU
Abstract: Methods and compositions are provided for assembly of large nucleic acids where the assembled large nucleic acids lack internal sequence modifications made during the assembly process.
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公开(公告)号:US20170081660A1
公开(公告)日:2017-03-23
申请号:US15268422
申请日:2016-09-16
Applicant: Twist Bioscience Corporation
Inventor: Anthony COX , Sebastian TREUSCH , Siyuan CHEN
IPC: C12N15/10 , C12N15/113 , C12Q1/68 , G01N33/50
CPC classification number: C12N15/1093 , C12N15/1079 , C12N15/113 , C12N2320/30 , C12N2330/31 , C12Q1/6876 , C12Q1/6886 , C12Q2600/158 , C40B50/08 , C40B50/14 , G01N33/502 , G01N33/5029 , G01N33/5041
Abstract: Disclosed herein are methods for the generation of highly accurate oligonucleic acid libraries encoding for predetermined variants of a nucleic acid sequence. The degree of variation may be complete, resulting in a saturated variant library, or less than complete, resulting in a selective library of variants. The variant oligonucleic acid libraries described herein may designed for further processing by transcription or translation. The variant oligonucleic acid libraries described herein may be designed to generate variant RNA, DNA and/or protein populations. Further provided herein are method for identifying variant species with increased or decreased activities, with applications in regulating biological functions and the design of therapeutics for treatment or reduction of disease.
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