Coordination of asparagine uptake and asparagine synthetase expression modulates CD8+ T cell activation

T cell receptor (TCR) triggering by antigen results in metabolic reprogramming that, in turn, facilitates the exit of T cells from quiescence. The increased nutrient requirements of activated lymphocytes are met, in part, by upregulation of cell surface transporters and enhanced uptake of amino acid...

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Main Authors: Helen Carrasco Hope, Rebecca J. Brownlie, Christopher M. Fife, Lynette Steele, Mihaela Lorger, Robert J. Salmond
Format: Article
Language:English
Published: American Society for Clinical investigation 2021-05-01
Series:JCI Insight
Subjects:
Online Access:https://doi.org/10.1172/jci.insight.137761
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spelling doaj-f09dbfc3ff2c45ebbd590954c6ced5e42021-08-02T22:14:52ZengAmerican Society for Clinical investigationJCI Insight2379-37082021-05-0169Coordination of asparagine uptake and asparagine synthetase expression modulates CD8+ T cell activationHelen Carrasco HopeRebecca J. BrownlieChristopher M. FifeLynette SteeleMihaela LorgerRobert J. SalmondT cell receptor (TCR) triggering by antigen results in metabolic reprogramming that, in turn, facilitates the exit of T cells from quiescence. The increased nutrient requirements of activated lymphocytes are met, in part, by upregulation of cell surface transporters and enhanced uptake of amino acids, fatty acids, and glucose from the environment. However, the role of intracellular pathways of amino acid biosynthesis in T cell activation is relatively unexplored. Asparagine is a nonessential amino acid that can be synthesized intracellularly through the glutamine-hydrolyzing enzyme asparagine synthetase (ASNS). We set out to define the requirements for uptake of extracellular asparagine and ASNS activity in CD8+ T cell activation. At early time points of activation in vitro, CD8+ T cells expressed little or no ASNS, and, as a consequence, viability and TCR-stimulated growth, activation, and metabolic reprogramming were substantially impaired under conditions of asparagine deprivation. At later time points (more than 24 hours of activation), TCR-induced mTOR-dependent signals resulted in ASNS upregulation that endowed CD8+ T cells with the capacity to function independently of extracellular asparagine. Thus, our data suggest that the coordinated upregulation of ASNS expression and uptake of extracellular asparagine is involved in optimal T cell effector responses.https://doi.org/10.1172/jci.insight.137761Immunology
collection DOAJ
language English
format Article
sources DOAJ
author Helen Carrasco Hope
Rebecca J. Brownlie
Christopher M. Fife
Lynette Steele
Mihaela Lorger
Robert J. Salmond
spellingShingle Helen Carrasco Hope
Rebecca J. Brownlie
Christopher M. Fife
Lynette Steele
Mihaela Lorger
Robert J. Salmond
Coordination of asparagine uptake and asparagine synthetase expression modulates CD8+ T cell activation
JCI Insight
Immunology
author_facet Helen Carrasco Hope
Rebecca J. Brownlie
Christopher M. Fife
Lynette Steele
Mihaela Lorger
Robert J. Salmond
author_sort Helen Carrasco Hope
title Coordination of asparagine uptake and asparagine synthetase expression modulates CD8+ T cell activation
title_short Coordination of asparagine uptake and asparagine synthetase expression modulates CD8+ T cell activation
title_full Coordination of asparagine uptake and asparagine synthetase expression modulates CD8+ T cell activation
title_fullStr Coordination of asparagine uptake and asparagine synthetase expression modulates CD8+ T cell activation
title_full_unstemmed Coordination of asparagine uptake and asparagine synthetase expression modulates CD8+ T cell activation
title_sort coordination of asparagine uptake and asparagine synthetase expression modulates cd8+ t cell activation
publisher American Society for Clinical investigation
series JCI Insight
issn 2379-3708
publishDate 2021-05-01
description T cell receptor (TCR) triggering by antigen results in metabolic reprogramming that, in turn, facilitates the exit of T cells from quiescence. The increased nutrient requirements of activated lymphocytes are met, in part, by upregulation of cell surface transporters and enhanced uptake of amino acids, fatty acids, and glucose from the environment. However, the role of intracellular pathways of amino acid biosynthesis in T cell activation is relatively unexplored. Asparagine is a nonessential amino acid that can be synthesized intracellularly through the glutamine-hydrolyzing enzyme asparagine synthetase (ASNS). We set out to define the requirements for uptake of extracellular asparagine and ASNS activity in CD8+ T cell activation. At early time points of activation in vitro, CD8+ T cells expressed little or no ASNS, and, as a consequence, viability and TCR-stimulated growth, activation, and metabolic reprogramming were substantially impaired under conditions of asparagine deprivation. At later time points (more than 24 hours of activation), TCR-induced mTOR-dependent signals resulted in ASNS upregulation that endowed CD8+ T cells with the capacity to function independently of extracellular asparagine. Thus, our data suggest that the coordinated upregulation of ASNS expression and uptake of extracellular asparagine is involved in optimal T cell effector responses.
topic Immunology
url https://doi.org/10.1172/jci.insight.137761
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