Pooled Knockin Targeting for Genome Engineering of Cellular Immunotherapies.
Citation | Roth, Theodore L, et al. “Pooled Knockin Targeting for Genome Engineering of Cellular Immunotherapies”. 2020. Cell, vol. 181, no. 3, 2020, pp. 728–744.e21. |
Author | Theodore L Roth, Jonathan Li, Franziska Blaeschke, Jasper F Nies, Ryan Apathy, Cody Mowery, Ruby Yu, Michelle L T Nguyen, Youjin Lee, Anna Truong, Joseph Hiatt, David Wu, David N Nguyen, Daniel Goodman, Jeffrey A Bluestone, Chun Jimmie Ye, Kole Roybal, Eric Shifrut, Alexander Marson |
Keywords | CRISPR, cell therapy, human T cell, knockins, pooled screen, single-cell RNA-seq |
Abstract |
Adoptive transfer of genetically modified immune cells holds great promise for cancer immunotherapy. CRISPR knockin targeting can improve cell therapies, but more high-throughput methods are needed to test which knockin gene constructs most potently enhance primary cell functions in vivo. We developed a widely adaptable technology to barcode and track targeted integrations of large non-viral DNA templates and applied it to perform pooled knockin screens in primary human T cells. Pooled knockin of dozens of unique barcoded templates into the T cell receptor (TCR)-locus revealed gene constructs that enhanced fitness in vitro and in vivo. We further developed pooled knockin sequencing (PoKI-seq), combining single-cell transcriptome analysis and pooled knockin screening to measure cell abundance and cell state ex vivo and in vivo. This platform nominated a novel transforming growth factor β (TGF-β) R2-41BB chimeric receptor that improved solid tumor clearance. Pooled knockin screening enables parallelized re-writing of endogenous genetic sequences to accelerate discovery of knockin programs for cell therapies. |
Year of Publication |
2020
|
Journal |
Cell
|
Volume |
181
|
Issue |
3
|
Number of Pages |
728-744.e21
|
Date Published |
04/2020
|
ISSN Number |
1097-4172
|
DOI |
10.1016/j.cell.2020.03.039
|
Alternate Journal |
Cell
|
PMID |
32302591
|
PMCID |
PMC7219528
|
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