alexa Peroxiredoxin-2 and STAT3 form a redox relay for H2O2 signaling.
Immunology

Immunology

Journal of Cell Signaling

Author(s): Sobotta MC, Liou W, Stcker S, Talwar D, Oehler M, , Sobotta MC, Liou W, Stcker S, Talwar D, Oehler M, , Sobotta MC, Liou W, Stcker S, Talwar D, Oehler M, , Sobotta MC, Liou W, Stcker S, Talwar D, Oehler M,

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Abstract Hydrogen peroxide (H(2)O(2)) acts as a signaling messenger by oxidatively modifying distinct cysteinyl thiols in distinct target proteins. However, it remains unclear how redox-regulated proteins, which often have low intrinsic reactivity towards H(2)O(2) (k(app) ∼1-10 M(-1) s(-1)), can be specifically and efficiently oxidized by H(2)O(2). Moreover, cellular thiol peroxidases, which are highly abundant and efficient H(2)O(2) scavengers, should effectively eliminate virtually all of the H(2)O(2) produced in the cell. Here, we show that the thiol peroxidase peroxiredoxin-2 (Prx2), one of the most H(2)O(2)-reactive proteins in the cell (k(app) ∼10(7)-10(8) M(-1) s(-1)), acts as a H(2)O(2) signal receptor and transmitter in transcription factor redox regulation. Prx2 forms a redox relay with the transcription factor STAT3 in which oxidative equivalents flow from Prx2 to STAT3. The redox relay generates disulfide-linked STAT3 oligomers with attenuated transcriptional activity. Cytokine-induced STAT3 signaling is accompanied by Prx2 and STAT3 oxidation and is modulated by Prx2 expression levels. This article was published in Nat Chem Biol and referenced in Journal of Cell Signaling

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