Wenjie Jin scite author profile

In response to pathogenic threats, naïve T cells rapidly transition from a quiescent to activated state, yet the underlying mechanisms are incompletely understood. Using a pulsed SILAC approach, we investigated the dynamics of mRNA translation kinetics and protein turnover in human naïve and activated T cells. Our datasets uncovered that transcription factors maintaining T cell quiescence had constitutively high turnover, which facilitated their depletion upon activation. Furthermore, naïve T cells maintained a surprisingly large number of idling ribosomes as well as 242 repressed mRNA species and a reservoir of glycolytic enzymes. These components were rapidly engaged following stimulation, promoting an immediate translational and glycolytic switch to ramp up the T cell activation program. Our data elucidate new insights into how T cells maintain a prepared state to mount a rapid immune response, and provide a resource of protein turnover, absolute translation kinetics and protein synthesis rates in T cells ( www.immunomics.ch ).

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Metabolic modulation of tumours with engineered bacteria for immunotherapy

Canale

Basso

Antonini

et al. 2021

Nature

307

193

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Spatial distribution and function of T follicular regulatory cells in human lymph nodes

et al. 2018

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Wenjie Jin

Dynamics in protein translation sustaining T cell preparedness

Metabolic modulation of tumours with engineered bacteria for immunotherapy

Spatial distribution and function of T follicular regulatory cells in human lymph nodes

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