Transcriptional and epigenetic regulators of human CD8 + T cell function identified through orthogonal CRISPR screens.
Sean R McCutcheonAdam M SwartzMichael C BrownAlejandro BarreraChristian McRoberts AmadorKeith SiklenkaLucas L HumayunMaria A Ter WeeleJames M IsaacsTimothy E ReddyAndrew S AllenSmita K NairScott J AntoniaCharles A GersbachPublished in: Nature genetics (2023)
Clinical response to adoptive T cell therapies is associated with the transcriptional and epigenetic state of the cell product. Thus, discovery of regulators of T cell gene networks and their corresponding phenotypes has potential to improve T cell therapies. Here we developed pooled, epigenetic CRISPR screening approaches to systematically profile the effects of activating or repressing 120 transcriptional and epigenetic regulators on human CD8 + T cell state. We found that BATF3 overexpression promoted specific features of memory T cells and attenuated gene programs associated with cytotoxicity, regulatory T cell function, and exhaustion. Upon chronic antigen stimulation, BATF3 overexpression countered phenotypic and epigenetic signatures of T cell exhaustion. Moreover, BATF3 enhanced the potency of CAR T cells in both in vitro and in vivo tumor models and programmed a transcriptional profile that correlates with positive clinical response to adoptive T cell therapy. Finally, we performed CRISPR knockout screens that defined cofactors and downstream mediators of the BATF3 gene network.
Keyphrases
- genome wide
- dna methylation
- cell therapy
- transcription factor
- gene expression
- copy number
- genome wide identification
- endothelial cells
- stem cells
- mesenchymal stem cells
- crispr cas
- genome editing
- induced pluripotent stem cells
- cell proliferation
- signaling pathway
- pluripotent stem cells
- public health
- risk assessment
- working memory
- oxidative stress
- network analysis