Targeted T cell receptor gene editing provides predictable T cell product function for immunotherapy Journal Article


Authors: Müller, T. R.; Jarosch, S.; Hammel, M.; Leube, J.; Grassmann, S.; Bernard, B.; Effenberger, M.; Andrä, I.; Chaudhry, M. Z.; Käuferle, T.; Malo, A.; Cicin-Sain, L.; Steinberger, P.; Feuchtinger, T.; Protzer, U.; Schumann, K.; Neuenhahn, M.; Schober, K.; Busch, D. H.
Article Title: Targeted T cell receptor gene editing provides predictable T cell product function for immunotherapy
Abstract: Adoptive transfer of T cells expressing a transgenic T cell receptor (TCR) has the potential to revolutionize immunotherapy of infectious diseases and cancer. However, the generation of defined TCR-transgenic T cell medicinal products with predictable in vivo function still poses a major challenge and limits broader and more successful application of this “living drug.” Here, by studying 51 different TCRs, we show that conventional genetic engineering by viral transduction leads to variable TCR expression and functionality as a result of variable transgene copy numbers and untargeted transgene integration. In contrast, CRISPR/Cas9-mediated TCR replacement enables defined, targeted TCR transgene insertion into the TCR gene locus. Thereby, T cell products display more homogeneous TCR expression similar to physiological T cells. Importantly, increased T cell product homogeneity after targeted TCR gene editing correlates with predictable in vivo T cell responses, which represents a crucial aspect for clinical application in adoptive T cell immunotherapy. © 2021 The Authors
Keywords: tcr; crispr/cas9 mediated engineering; homogenous tcr expreession; orthotopic tcr replacement; otr; predictable functionality; t cell receptor engineering; tcr editing; tcr transgenic t cells
Journal Title: Cell Reports Medicine
Volume: 2
Issue: 8
ISSN: 2666-3791
Publisher: Cell Press  
Date Published: 2021-08-17
Start Page: 100374
Language: English
DOI: 10.1016/j.xcrm.2021.100374
PROVIDER: scopus
PMCID: PMC8385324
PUBMED: 34467251
DOI/URL:
Notes: Article -- Export Date: 1 September 2021 -- Source: Scopus
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