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Sodium perturbs mitochondrial respiration and induces dysfunctional Tregs

Authors :
Côrte-Real, Beatriz F.
Hamad, Ibrahim
Arroyo Hornero, Rebeca
Geisberger, Sabrina
Roels, Joris
Van Zeebroeck, Lauren
Dyczko, Aleksandra
van Gisbergen, Marike W.
Kurniawan, Henry
Wagner, Allon
Yosef, Nir
Weiss, Susanne N.Y.
Schmetterer, Klaus G.
Schröder, Agnes
Krampert, Luka
Haase, Stefanie
Bartolomaeus, Hendrik
Hellings, Niels
Saeys, Yvan
Dubois, Ludwig J.
Brenner, Dirk
Kempa, Stefan
Hafler, David A.
Stegbauer, Johannes
Linker, Ralf A.
Jantsch, Jonathan
Müller, Dominik N.
Kleinewietfeld, Markus
Côrte-Real, Beatriz F.
Hamad, Ibrahim
Arroyo Hornero, Rebeca
Geisberger, Sabrina
Roels, Joris
Van Zeebroeck, Lauren
Dyczko, Aleksandra
van Gisbergen, Marike W.
Kurniawan, Henry
Wagner, Allon
Yosef, Nir
Weiss, Susanne N.Y.
Schmetterer, Klaus G.
Schröder, Agnes
Krampert, Luka
Haase, Stefanie
Bartolomaeus, Hendrik
Hellings, Niels
Saeys, Yvan
Dubois, Ludwig J.
Brenner, Dirk
Kempa, Stefan
Hafler, David A.
Stegbauer, Johannes
Linker, Ralf A.
Jantsch, Jonathan
Müller, Dominik N.
Kleinewietfeld, Markus
Source :
Cell Metabolism vol.35 (2023) date: 2023-02-07 nr.2 p.299-315.e8 [ISSN 1550-4131]
Publication Year :
2023

Abstract

FOXP3+ regulatory T cells (Tregs) are central for peripheral tolerance, and their deregulation is associated with autoimmunity. Dysfunctional autoimmune Tregs display pro-inflammatory features and altered mitochondrial metabolism, but contributing factors remain elusive. High salt (HS) has been identified to alter immune function and to promote autoimmunity. By investigating longitudinal transcriptional changes of human Tregs, we identified that HS induces metabolic reprogramming, recapitulating features of autoimmune Tregs. Mechanistically, extracellular HS raises intracellular Na+, perturbing mitochondrial respiration by interfering with the electron transport chain (ETC). Metabolic disturbance by a temporary HS encounter or complex III blockade rapidly induces a pro-inflammatory signature and FOXP3 downregulation, leading to long-term dysfunction in vitro and in vivo. The HS-induced effect could be reversed by inhibition of mitochondrial Na+/Ca2+ exchanger (NCLX). Our results indicate that salt could contribute to metabolic reprogramming and that short-term HS encounter perturb metabolic fitness and long-term function of human Tregs with important implications for autoimmunity.

Details

Database :
OAIster
Journal :
Cell Metabolism vol.35 (2023) date: 2023-02-07 nr.2 p.299-315.e8 [ISSN 1550-4131]
Notes :
DOI: 10.1016/j.cmet.2023.01.009, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1427435643
Document Type :
Electronic Resource