Metabolic and epigenetic regulation of T-cell exhaustion

Current immunotherapies yield remarkable clinical outcomes by boosting the power of host immunity in cancer cell elimination and viral clearance. However, after prolonged antigen exposure, CD8 + T cells differentiate into a special differentiation state known as T-cell exhaustion, which poses one of...

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Veröffentlicht in:Nature metabolism 2020-10, Vol.2 (10), p.1001-1012
Hauptverfasser: Franco, Fabien, Jaccard, Alison, Romero, Pedro, Yu, Yi-Ru, Ho, Ping-Chih
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Sprache:eng
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Zusammenfassung:Current immunotherapies yield remarkable clinical outcomes by boosting the power of host immunity in cancer cell elimination and viral clearance. However, after prolonged antigen exposure, CD8 + T cells differentiate into a special differentiation state known as T-cell exhaustion, which poses one of the major hurdles to antiviral and antitumor immunity during chronic viral infection and tumour development. Growing evidence indicates that exhausted T cells undergo metabolic insufficiency with altered signalling cascades and epigenetic landscapes, which dampen effector immunity and cause poor responsiveness to immune-checkpoint-blockade therapies. How metabolic stress affects T-cell exhaustion remains unclear; therefore, in this Review, we summarize current knowledge of how T-cell exhaustion occurs, and discuss how metabolic insufficiency and prolonged stress responses may affect signalling cascades and epigenetic reprogramming, thus locking T cells into an exhausted state via specialized differentiation programming. Franco et al, review how metabolic insufficiency and prolonged stress responses impact signaling cascades and epigenetic reprogramming to lock T cells into an exhausted state.
ISSN:2522-5812
2522-5812
DOI:10.1038/s42255-020-00280-9