Mitigation of chromosome loss in clinical CRISPR-Cas9-engineered T cells.
Connor A TsuchidaNadav BrandesRaymund BuenoMarena I TrinidadThomas MazumderBingfei YuByungjin HwangChristopher ChangJamin LiuYang SunCaitlin R HopkinsKevin R ParkerYanyan QiAnsuman T SatpathyEdward A StadtmauerJamie H D CateJustin EyquemJoseph A FraiettaCarl H JuneHoward Y ChangChun Jimmie YeJennifer A DoudnaPublished in: bioRxiv : the preprint server for biology (2023)
CRISPR-Cas9 genome editing has enabled advanced T cell therapies, but occasional loss of the targeted chromosome remains a safety concern. To investigate whether Cas9-induced chromosome loss is a universal phenomenon and evaluate its clinical significance, we conducted a systematic analysis in primary human T cells. Arrayed and pooled CRISPR screens revealed that chromosome loss was generalizable across the genome and resulted in partial and entire loss of the chromosome, including in pre-clinical chimeric antigen receptor T cells. T cells with chromosome loss persisted for weeks in culture, implying the potential to interfere with clinical use. A modified cell manufacturing process, employed in our first-in-human clinical trial of Cas9-engineered T cells, 1 dramatically reduced chromosome loss while largely preserving genome editing efficacy. Expression of p53 correlated with protection from chromosome loss observed in this protocol, suggesting both a mechanism and strategy for T cell engineering that mitigates this genotoxicity in the clinic.