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T cells at work: How post‐transcriptional mechanisms control T cell homeostasis and activation

Anouk P. Jurgens, Branka Popović, Monika C. Wolkers

2021European Journal of Immunology47 citationsDOIOpen Access PDF

Abstract

T cells are central players of the adaptive immune system by protecting us from recurring infections and by killing malignant cells. Protective T cell responses rely on the concerted production of effector molecules such as cytolytic mediators, granzymes, and perforins, as well as pro-inflammatory cytokines and chemokines. Once activated, T cells drastically change their gene expression and rapidly respond to insults by producing ample amounts of effector molecules. In the absence of antigen, T cells remain in a quiescent state and survey our body for possible pathogenic insults. Resting T cells are, however, not inert, but continuously regulate their protein production to survive and to be prepared for possible re-infections. Here, we review our current knowledge on the regulation of gene expression in activated and quiescent T cells. We specifically focus on post-transcriptional mechanisms that define the protein output and that allow dormant cells to undergo active signaling and selective translation, keeping them poised for activation. Finally, we discuss which signals drive T cell survival and their preparedness to respond to insults and which mechanisms are involved in these processes.

Topics & Concepts

BiologyCell biologyEffectorChemokineImmune systemT cellAntigen-presenting cellAcquired immune systemImmunologyImmune Cell Function and InteractionT-cell and B-cell ImmunologyCAR-T cell therapy research
T cells at work: How post‐transcriptional mechanisms control T cell homeostasis and activation | Litcius