AI Article Synopsis
- T cell senescence and exhaustion limit the effectiveness of cancer immunotherapy.
- The study demonstrates that miR-155 boosts CD8 T cell function against tumors by preventing senescence and exhaustion through the suppression of certain differentiation drivers.
- It highlights a key mechanism involving miR-155, Phf19, and the Polycomb repressor complex 2 (PRC2) that together help maintain CD8 T cell activity and differentiation, suggesting potential for enhancing cancer treatments through epigenetic strategies.
Article Abstract
T cell senescence and exhaustion are major barriers to successful cancer immunotherapy. Here we show that miR-155 increases CD8 T cell antitumor function by restraining T cell senescence and functional exhaustion through epigenetic silencing of drivers of terminal differentiation. miR-155 enhances Polycomb repressor complex 2 (PRC2) activity indirectly by promoting the expression of the PRC2-associated factor Phf19 through downregulation of the Akt inhibitor, Ship1. Phf19 orchestrates a transcriptional program extensively shared with miR-155 to restrain T cell senescence and sustain CD8 T cell antitumor responses. These effects rely on Phf19 histone-binding capacity, which is critical for the recruitment of PRC2 to the target chromatin. These findings establish the miR-155-Phf19-PRC2 as a pivotal axis regulating CD8 T cell differentiation, thereby paving new ways for potentiating cancer immunotherapy through epigenetic reprogramming of CD8 T cell fate.
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Source |
|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6517388 | PMC |
| http://dx.doi.org/10.1038/s41467-019-09882-8 | DOI Listing |
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