公开(公告)号：US20170114406A1

公开(公告)日：2017-04-27

申请号：US15312909

申请日：2015-05-22

申请人： THE UNIVERSITY OF BRITISH COLUMBIA

发明人： Carl Lars, Genghis HANSEN ,  Georgia Elizabeth MEWIS ,  Kevin Albert HEYRIES ,  Michael Andrew VANINSBERGHE ,  Daniel Jay DA COSTA ,  Marketa RICICOVA

IPC分类号： C12Q1/68 ,  G06F19/22 ,  G06F19/24

CPC分类号： C12Q1/6876 ,  C07K14/7051 ,  C12Q2600/158 ,  C40B20/00 ,  C40B30/04 ,  G01N33/68 ,  G16B30/00 ,  G16B40/00 ,  C12Q2535/122

摘要： Provided herein are high-throughput sequencing methods to study the diversity and functionality of lymphocyte receptor chains and pairing of the same. Specifically, the methods provided herein are used to identify with confidence one or more lymphocyte receptor chain pairs in a sample, for example one or more functional chain pairs.

公开(公告)号：US20190300954A1

公开(公告)日：2019-10-03

申请号：US16423861

申请日：2019-05-28

申请人： THE UNIVERSITY OF BRITISH COLUMBIA

发明人： Carl Lars Genghis HANSEN ,  Georgia Elizabeth MEWIS ,  Kevin Albert HEYRIES ,  Michael Andrew VANINSBERGHE ,  Daniel Jay DA COSTA ,  Marketa RICICOVA

IPC分类号： C12Q1/6876 ,  G16B40/00 ,  G16B30/00 ,  C07K14/725 ,  C40B20/00 ,  G01N33/68

摘要： Provided herein are high-throughput sequencing methods to study the diversity and functionality of lymphocyte receptor chains and pairing of the same. Specifically, the methods provided herein are used to identify with confidence one or more lymphocyte receptor chain pairs in a sample, for example one or more functional chain pairs.

公开(公告)号：US20230041481A1

公开(公告)日：2023-02-09

申请号：US17835220

申请日：2022-06-08

申请人： The University of British Columbia

发明人： Carl Lars Genghis HANSEN ,  Georgia Elizabeth MEWIS ,  Kevin Albert HEYRIES ,  Michael Andrew VANINSBERGHE ,  Daniel Jay DA COSTA ,  Marketa RICICOVA

IPC分类号： C40B30/04 ,  G16B30/00 ,  G16B40/00 ,  C40B20/00 ,  G01N33/68 ,  C07K14/725 ,  G16B30/20 ,  G16B30/10 ,  C12Q1/6876

摘要： Provided herein are high-throughput sequencing methods to study the diversity and functionality of lymphocyte receptor chains and pairing of the same. Specifically, the methods provided herein are used to identify with confidence one or more lymphocyte receptor chain pairs in a sample, for example one or more functional chain pairs.

公开(公告)号：US20210269792A1

公开(公告)日：2021-09-02

申请号：US17321645

申请日：2021-05-17

申请人： THE UNIVERSITY OF BRITISH COLUMBIA

发明人： Ester FALCONER ,  Carl Lars Genghis HANSEN ,  Veronique LECAULT ,  Kathleen LISAINGO ,  Kevin Albert HEYRIES

IPC分类号： C12N15/10 ,  C12Q1/6874 ,  G01N33/566 ,  G01N33/68

摘要： The present invention relates to methods for isolating the sequences of an antibody that reacts with a disease related antigen, e.g., an autoantigen, without knowing the identity of the antigen (sequence or structural epitope) a priori. The methods can also be used to identify an antigen that mediates a disease state, e.g., an autoantigen implicated in an autoimmune disorder or a tumor response.

公开(公告)号：US20220365072A1

公开(公告)日：2022-11-17

申请号：US17369425

申请日：2021-07-07

申请人： The University of British Columbia

发明人： Marketa RICICOVA ,  Kevin Albert HEYRIES ,  Hans ZAHN ,  Oleh PETRIV ,  Veronique LECAULT ,  Anupam Singhal ,  Daniel J. Da Costa ,  Carl L. G. Hansen ,  Brad NELSON ,  Julie NIELSEN ,  Kathleen Lisaingo

IPC分类号： G01N33/50 ,  B01L3/00 ,  C07K16/40 ,  G01N33/543 ,  C07K16/10 ,  C07K16/00 ,  C12N5/078 ,  C12N5/0781 ,  C12Q1/6888 ,  G01N33/68 ,  G01N35/00

摘要： Methods and devices are provided herein for identifying a cell population comprising an effector cell that exerts an extracellular effect. In one embodiment the method comprises retaining in a microreactor a cell population comprising one or more effector cells, wherein the contents of the microreactor further comprise a readout particle population comprising one or more readout particles, incubating the cell population and the readout particle population within the microreactor, assaying the cell population for the presence of the extracellular effect, wherein the readout particle population or subpopulation thereof provides a direct or indirect readout of the extracellular effect, and determining, based on the results of the assaying step, whether one or more effector cells within the cell population exerts the extracellular effect on the readout particle. If an extracellular effect is measured, the cell population is recovered for further analysis to determine the cell or cells responsible for the effect.

公开(公告)号：US20200149031A1

公开(公告)日：2020-05-14

申请号：US16063394

申请日：2016-12-21

申请人： THE UNIVERSITY OF BRITISH COLUMBIA

发明人： Ester FALCONER ,  Carl Lars Genghis HANSEN ,  Veronique LECAULT ,  Kathleen LISAINGO ,  Kevin Albert HEYRIES

IPC分类号： C12N15/10 ,  G01N33/566 ,  G01N33/68 ,  C12Q1/6874

摘要： The present invention relates to methods for isolating the sequences of an antibody that reacts with a disease related antigen, e.g., an autoantigen, without knowing the identity of the antigen (sequence or structural epitope) a priori. The methods can also be used to identify an antigen that mediates a disease state, e.g., an autoantigen implicated in an autoimmune disorder or a tumor response.