| Literature DB >> 35773341 |
Alessio David Nahmad1,2, Eli Reuveni3, Ella Goldschmidt4, Tamar Tenne5, Meytal Liberman5, Miriam Horovitz-Fried1,2, Rami Khosravi6, Hila Kobo7, Eyal Reinstein5,8, Asaf Madi9, Uri Ben-David10, Adi Barzel11,12.
Abstract
Multiple clinical trials of allogeneic T cell therapy use site-specific nucleases to disrupt T cell receptor (TCR) and other genes1-6. In this study, using single-cell RNA sequencing, we investigated genome editing outcomes in primary human T cells transfected with CRISPR-Cas9 and guide RNAs targeting genes for TCR chains and programmed cell death protein 1. Four days after transfection, we found a loss of chromosome 14, harboring the TCRα locus, in up to 9% of the cells and a chromosome 14 gain in up to 1.4% of the cells. Chromosome 7, harboring the TCRβ locus, was truncated in 9.9% of the cells. Aberrations were validated using fluorescence in situ hybridization and digital droplet PCR. Aneuploidy was associated with reduced proliferation, induced p53 activation and cell death. However, at 11 days after transfection, 0.9% of T cells still had a chromosome 14 loss. Aneuploidy and chromosomal truncations are, thus, frequent outcomes of CRISPR-Cas9 cleavage that should be monitored and minimized in clinical protocols.Entities:
Year: 2022 PMID: 35773341 DOI: 10.1038/s41587-022-01377-0
Source DB: PubMed Journal: Nat Biotechnol ISSN: 1087-0156 Impact factor: 54.908