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Efficient isolation of rare B cells using next-generation antigen barcoding.


ABSTRACT: The ability to efficiently isolate antigen-specific B cells in high throughput will greatly accelerate the discovery of therapeutic monoclonal antibodies (mAbs) and catalyze rational vaccine development. Traditional mAb discovery is a costly and labor-intensive process, although recent advances in single-cell genomics using emulsion microfluidics allow simultaneous processing of thousands of individual cells. Here we present a streamlined method for isolation and analysis of large numbers of antigen-specific B cells, including next generation antigen barcoding and an integrated computational framework for B cell multi-omics. We demonstrate the power of this approach by recovering thousands of antigen-specific mAbs, including the efficient isolation of extremely rare precursors of VRC01-class and IOMA-class broadly neutralizing HIV mAbs.

SUBMITTER: Hurtado J 

PROVIDER: S-EPMC10036767 | biostudies-literature | 2022

REPOSITORIES: biostudies-literature

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Efficient isolation of rare B cells using next-generation antigen barcoding.

Hurtado Jonathan J   Flynn Claudia C   Lee Jeong Hyun JH   Salcedo Eugenia C EC   Cottrell Christopher A CA   Skog Patrick D PD   Burton Dennis R DR   Nemazee David D   Schief William R WR   Landais Elise E   Sok Devin D   Briney Bryan B  

Frontiers in cellular and infection microbiology 20230310


The ability to efficiently isolate antigen-specific B cells in high throughput will greatly accelerate the discovery of therapeutic monoclonal antibodies (mAbs) and catalyze rational vaccine development. Traditional mAb discovery is a costly and labor-intensive process, although recent advances in single-cell genomics using emulsion microfluidics allow simultaneous processing of thousands of individual cells. Here we present a streamlined method for isolation and analysis of large numbers of ant  ...[more]

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