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. 2025 Jun;7(6):1183-1203.
doi: 10.1038/s42255-025-01275-0. Epub 2025 Apr 18.

Itaconate modulates immune responses via inhibition of peroxiredoxin 5

Tomas Paulenda  1 Barbora Echalar  1 Lucie Potuckova  1 Veronika Vachova  1 Denis A Kleverov  1 Johannes Mehringer  2   3 Ekaterina Potekhina  4   5 Alex Jacoby  6 Devashish Sen  1 Chris Nelson  1 Rick Stegeman  1 Vladimir Sukhov  1 Danielle Kemper  6 Cheryl F Lichti  1   7 Nicholas J Day  8 Tong Zhang  8 Kamila Husarcikova  1 Monika Bambouskova  9 Daved H Fremont  1   10   11 Wei-Jun Qian  8 Sergej Djuranovic  6 Slavica Pavlovic-Djuranovic  6 Vsevolod V Belousov  4   5 Andrzej M Krezel  10 Maxim N Artyomov  12
Affiliations

Itaconate modulates immune responses via inhibition of peroxiredoxin 5

Tomas Paulenda et al. Nat Metab. 2025 Jun.

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.

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Conflict of interest statement

Competing interests: The authors declare no competing interests.

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