Itaconate modulates immune responses via inhibition of peroxiredoxin 5

Tomas Paulenda; Barbora Echalar; Lucie Potuckova; Veronika Vachova; Denis A. Kleverov; Johannes Mehringer; Ekaterina Potekhina; Alex Jacoby; Devashish Sen; Chris Nelson; Rick Stegeman; Vladimir Sukhov; Danielle Kemper; Cheryl F. Lichti; Nicholas J. Day; Tong Zhang; Kamila Husarcikova; Monika Bambouskova; Daved H. Fremont; Wei Jun Qian; Sergej Djuranovic; Slavica Pavlovic-Djuranovic; Vsevolod V. Belousov; Andrzej M. Krezel; Maxim N. Artyomov

doi:10.1038/s42255-025-01275-0

Itaconate modulates immune responses via inhibition of peroxiredoxin 5

Tomas Paulenda, Barbora Echalar, Lucie Potuckova, Veronika Vachova, Denis A. Kleverov, Johannes Mehringer, Ekaterina Potekhina, Alex Jacoby, Devashish Sen, Chris Nelson, Rick Stegeman, Vladimir Sukhov, Danielle Kemper, Cheryl F. Lichti, Nicholas J. Day, Tong Zhang, Kamila Husarcikova, Monika Bambouskova, Daved H. Fremont, Wei Jun QianSergej Djuranovic, Slavica Pavlovic-Djuranovic, Vsevolod V. Belousov, Andrzej M. Krezel, Maxim N. Artyomov

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Abstract

The immunoregulatory metabolite itaconate accumulates in innate immune cells upon Toll-like receptor stimulation. In response to macrophage activation by lipopolysaccharide, itaconate inhibits inflammasome activation and boosts type I interferon signalling; however, the molecular mechanism of this immunoregulation remains unclear. Here, we show that the enhancement of type I interferon secretion by itaconate depends on the inhibition of peroxiredoxin 5 and on mitochondrial reactive oxygen species. We find that itaconate non-covalently inhibits peroxiredoxin 5, leading to the modulation of mitochondrial peroxide in activating macrophages. Through genetic manipulation, we confirm that peroxiredoxin 5 modulates type I interferon secretion in macrophages. The non-electrophilic itaconate mimetic 2-methylsuccinate inhibits peroxiredoxin 5 and phenocopies immunoregulatory action of itaconate on type I interferon and inflammasome activation, providing further support for a non-covalent inhibition of peroxiredoxin 5 by itaconate. Our work provides insight into the molecular mechanism of actions and biological rationale for the predominantly immune specification of itaconate.

Original language	English
Article number	3513
Journal	Nature Metabolism
DOIs	https://doi.org/10.1038/s42255-025-01275-0
State	Accepted/In press - 2025

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Paulenda, T., Echalar, B., Potuckova, L., Vachova, V., Kleverov, D. A., Mehringer, J., Potekhina, E., Jacoby, A., Sen, D., Nelson, C., Stegeman, R., Sukhov, V., Kemper, D., Lichti, C. F., Day, N. J., Zhang, T., Husarcikova, K., Bambouskova, M., Fremont, D. H., ... Artyomov, M. N. (Accepted/In press). Itaconate modulates immune responses via inhibition of peroxiredoxin 5. Nature Metabolism, Article 3513. https://doi.org/10.1038/s42255-025-01275-0

@article{2407c04be2a84485aa824cb6cf5a6ed1,

title = "Itaconate modulates immune responses via inhibition of peroxiredoxin 5",

abstract = "The immunoregulatory metabolite itaconate accumulates in innate immune cells upon Toll-like receptor stimulation. In response to macrophage activation by lipopolysaccharide, itaconate inhibits inflammasome activation and boosts type I interferon signalling; however, the molecular mechanism of this immunoregulation remains unclear. Here, we show that the enhancement of type I interferon secretion by itaconate depends on the inhibition of peroxiredoxin 5 and on mitochondrial reactive oxygen species. We find that itaconate non-covalently inhibits peroxiredoxin 5, leading to the modulation of mitochondrial peroxide in activating macrophages. Through genetic manipulation, we confirm that peroxiredoxin 5 modulates type I interferon secretion in macrophages. The non-electrophilic itaconate mimetic 2-methylsuccinate inhibits peroxiredoxin 5 and phenocopies immunoregulatory action of itaconate on type I interferon and inflammasome activation, providing further support for a non-covalent inhibition of peroxiredoxin 5 by itaconate. Our work provides insight into the molecular mechanism of actions and biological rationale for the predominantly immune specification of itaconate.",

author = "Tomas Paulenda and Barbora Echalar and Lucie Potuckova and Veronika Vachova and Kleverov, {Denis A.} and Johannes Mehringer and Ekaterina Potekhina and Alex Jacoby and Devashish Sen and Chris Nelson and Rick Stegeman and Vladimir Sukhov and Danielle Kemper and Lichti, {Cheryl F.} and Day, {Nicholas J.} and Tong Zhang and Kamila Husarcikova and Monika Bambouskova and Fremont, {Daved H.} and Qian, {Wei Jun} and Sergej Djuranovic and Slavica Pavlovic-Djuranovic and Belousov, {Vsevolod V.} and Krezel, {Andrzej M.} and Artyomov, {Maxim N.}",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature Limited 2025.",

year = "2025",

doi = "10.1038/s42255-025-01275-0",

language = "English",

journal = "Nature Metabolism",

issn = "2522-5812",

}

Paulenda, T, Echalar, B, Potuckova, L, Vachova, V, Kleverov, DA, Mehringer, J, Potekhina, E, Jacoby, A, Sen, D, Nelson, C, Stegeman, R, Sukhov, V, Kemper, D, Lichti, CF, Day, NJ, Zhang, T, Husarcikova, K, Bambouskova, M , Fremont, DH, Qian, WJ, Djuranovic, S , Pavlovic-Djuranovic, S, Belousov, VV, Krezel, AM & Artyomov, MN 2025, 'Itaconate modulates immune responses via inhibition of peroxiredoxin 5', Nature Metabolism. https://doi.org/10.1038/s42255-025-01275-0

TY - JOUR

T1 - Itaconate modulates immune responses via inhibition of peroxiredoxin 5

AU - Paulenda, Tomas

AU - Echalar, Barbora

AU - Potuckova, Lucie

AU - Vachova, Veronika

AU - Kleverov, Denis A.

AU - Mehringer, Johannes

AU - Potekhina, Ekaterina

AU - Jacoby, Alex

AU - Sen, Devashish

AU - Nelson, Chris

AU - Stegeman, Rick

AU - Sukhov, Vladimir

AU - Kemper, Danielle

AU - Lichti, Cheryl F.

AU - Day, Nicholas J.

AU - Zhang, Tong

AU - Husarcikova, Kamila

AU - Bambouskova, Monika

AU - Fremont, Daved H.

AU - Qian, Wei Jun

AU - Djuranovic, Sergej

AU - Pavlovic-Djuranovic, Slavica

AU - Belousov, Vsevolod V.

AU - Krezel, Andrzej M.

AU - Artyomov, Maxim N.

PY - 2025

Y1 - 2025

N2 - The immunoregulatory metabolite itaconate accumulates in innate immune cells upon Toll-like receptor stimulation. In response to macrophage activation by lipopolysaccharide, itaconate inhibits inflammasome activation and boosts type I interferon signalling; however, the molecular mechanism of this immunoregulation remains unclear. Here, we show that the enhancement of type I interferon secretion by itaconate depends on the inhibition of peroxiredoxin 5 and on mitochondrial reactive oxygen species. We find that itaconate non-covalently inhibits peroxiredoxin 5, leading to the modulation of mitochondrial peroxide in activating macrophages. Through genetic manipulation, we confirm that peroxiredoxin 5 modulates type I interferon secretion in macrophages. The non-electrophilic itaconate mimetic 2-methylsuccinate inhibits peroxiredoxin 5 and phenocopies immunoregulatory action of itaconate on type I interferon and inflammasome activation, providing further support for a non-covalent inhibition of peroxiredoxin 5 by itaconate. Our work provides insight into the molecular mechanism of actions and biological rationale for the predominantly immune specification of itaconate.

AB - The immunoregulatory metabolite itaconate accumulates in innate immune cells upon Toll-like receptor stimulation. In response to macrophage activation by lipopolysaccharide, itaconate inhibits inflammasome activation and boosts type I interferon signalling; however, the molecular mechanism of this immunoregulation remains unclear. Here, we show that the enhancement of type I interferon secretion by itaconate depends on the inhibition of peroxiredoxin 5 and on mitochondrial reactive oxygen species. We find that itaconate non-covalently inhibits peroxiredoxin 5, leading to the modulation of mitochondrial peroxide in activating macrophages. Through genetic manipulation, we confirm that peroxiredoxin 5 modulates type I interferon secretion in macrophages. The non-electrophilic itaconate mimetic 2-methylsuccinate inhibits peroxiredoxin 5 and phenocopies immunoregulatory action of itaconate on type I interferon and inflammasome activation, providing further support for a non-covalent inhibition of peroxiredoxin 5 by itaconate. Our work provides insight into the molecular mechanism of actions and biological rationale for the predominantly immune specification of itaconate.

UR - http://www.scopus.com/inward/record.url?scp=105003052778&partnerID=8YFLogxK

U2 - 10.1038/s42255-025-01275-0

DO - 10.1038/s42255-025-01275-0

M3 - Article

AN - SCOPUS:105003052778

SN - 2522-5812

JO - Nature Metabolism

JF - Nature Metabolism

M1 - 3513

ER -

Itaconate modulates immune responses via inhibition of peroxiredoxin 5

Abstract

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