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  5. CD8<sup>+</sup> T-Cell Metabolic Rewiring Defined by Single-Cell RNA-Sequencing Identifies a Critical Role of ASNS Expression Dynamics in T-Cell Differentiation

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Preprint
en
2021

CD8<sup>+</sup> T-Cell Metabolic Rewiring Defined by Single-Cell RNA-Sequencing Identifies a Critical Role of ASNS Expression Dynamics in T-Cell Differentiation

0 Datasets

0 Files

en
2021
DOI: 10.1101/2021.07.27.453976

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Peter Carmeliet
Peter Carmeliet

Aarhus University

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Juan Fernández-García
Fabien Franco
Sweta Parik
+12 more

Abstract

ABSTRACT Cytotoxic T cells dynamically rewire their metabolism during the course of an immune response. While T-cell metabolism has been extensively studied at phenotypic endpoints of activation and differentiation, the underlying dynamics remain largely elusive. Here, we leverage on single-cell RNA-sequencing (scRNA-seq) measurements of in vitro activated and differentiated CD8 + T cells cultured in physiological media to resolve these metabolic dynamics. We find that our scRNA-seq analysis identifies most metabolic changes previously defined in in vivo experiments, such as a rewiring from an oxidative to an anabolism-promoting metabolic program during activation to an effector state, which is later reverted upon memory polarization. Importantly, our scRNA-seq data further provide a dynamic description of these changes. In this sense, our data predict a differential time-dependent reliance of CD8 + T cells on the synthesis versus uptake of various non-essential amino acids during T-cell activation, which we corroborate with additional functional in vitro experiments. We further exploit our scRNA-seq data to identify metabolic genes that could potentially dictate the outcome of T-cell differentiation, by ranking them based on their expression dynamics. Among the highest-ranked hits, we find asparagine synthetase ( Asns ), whose expression sharply peaks for effector CD8 + T cells and further decays towards memory polarization. We then confirm that these in vitro Asns expression dynamics are representative of an in vivo situation in a mouse model of viral infection. Moreover, we find that disrupting these expression dynamics in vitro , by depleting asparagine from the culture media, delays central-memory polarization. Accordingly, we find that preventing the decay of ASNS by stable overexpression at the protein level in vivo leads to a significant increase in effector CD8 + T-cell expansion, and a concomitant decrease in central-memory formation, in a mouse model of viral infection. This shows that ASNS expression dynamics dictate the fate of CD8 + T-cell differentiation. In conclusion, we provide a resource of dynamic expression changes during CD8 + T-cell activation and differentiation that is expected to increase our understanding of the dynamic metabolic requirements of T cells progressing along the immune response cascade.

How to cite this publication

Juan Fernández-García, Fabien Franco, Sweta Parik, Antonino Alejandro Pane, Dorien Broekaert, Joke Van Elsen, Ines Vermeire, Thomas Van Brussel, Rogier Schepers, Elodie Modave, Tobias K. Karakach, Peter Carmeliet, Diether Lambrechts, Ping‐Chih Ho, Sarah‐Maria Fendt (2021). CD8<sup>+</sup> T-Cell Metabolic Rewiring Defined by Single-Cell RNA-Sequencing Identifies a Critical Role of ASNS Expression Dynamics in T-Cell Differentiation. , DOI: https://doi.org/10.1101/2021.07.27.453976.

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Publication Details

Type

Preprint

Year

2021

Authors

15

Datasets

0

Total Files

0

Language

en

DOI

https://doi.org/10.1101/2021.07.27.453976

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