Cysteine Oxidation Targets Peroxiredoxins 1 and 2 for Exosomal Release through a Novel Mechanism of Redox-Dependent Secretion

“…Their findings suggest the existence of a protein export system that specifically recognizes glutathionylated proteins including Prx2. The authors recently characterized the role of exosomes for the release of Prx1 and Prx2 [28]. Treatment of HEK cells and monocytic cells with either LPS or TNF-α enhanced secretion of disulphide-linked homodimers of Prx1 and Prx2 [28] (Figs.…”

“…The mechanisms and roles of Prx1 and Prx2 secretion from cells through exosomes should be underscored [28]. Exosomes are small vesicle generated in the endosomal structure and released from various cells.…”

“…The glutathionylation at Cys83 stabilizes the dimer structure [42]. Prx1 and also Prx2 can be secreted from cells associated with exosomes [28,45]. (B) Interaction of Prx1 with TLR4 requires serum components.…”

“…PPAR-γ directly interacts with NF-κB and inhibits its DNA binding [9][10][11][12][13]. their S-glutathionylated dimer forms associated with exosomes [28,45]. [99,100].…”

“…Prx1 is also detected in mouse body fluids, and the secretion of Prx1 from cultured cells was enhanced following the treatment with cytokines such as TGF-β, oncostatin M and IL1-β (reviewed in [27]). A recent study show Prx1 and Prx2 can be secreted from cells as disulphide homodimers in association with exosomes following stimulation by LPS or TNF-α [28]. A previous study demonstrated importance of Prx1 in the initiation of pulmonary inflammation following exposure to non-lethal levels of ozone [29].…”

Close teamwork between Nrf2 and peroxiredoxins 1 and 6 for the regulation of prostaglandin D2 and E2 production in macrophages in acute inflammation

“…Their findings suggest the existence of a protein export system that specifically recognizes glutathionylated proteins including Prx2. The authors recently characterized the role of exosomes for the release of Prx1 and Prx2 [28]. Treatment of HEK cells and monocytic cells with either LPS or TNF-α enhanced secretion of disulphide-linked homodimers of Prx1 and Prx2 [28] (Figs.…”

“…The mechanisms and roles of Prx1 and Prx2 secretion from cells through exosomes should be underscored [28]. Exosomes are small vesicle generated in the endosomal structure and released from various cells.…”

“…The glutathionylation at Cys83 stabilizes the dimer structure [42]. Prx1 and also Prx2 can be secreted from cells associated with exosomes [28,45]. (B) Interaction of Prx1 with TLR4 requires serum components.…”

“…PPAR-γ directly interacts with NF-κB and inhibits its DNA binding [9][10][11][12][13]. their S-glutathionylated dimer forms associated with exosomes [28,45]. [99,100].…”

“…Prx1 is also detected in mouse body fluids, and the secretion of Prx1 from cultured cells was enhanced following the treatment with cytokines such as TGF-β, oncostatin M and IL1-β (reviewed in [27]). A recent study show Prx1 and Prx2 can be secreted from cells as disulphide homodimers in association with exosomes following stimulation by LPS or TNF-α [28]. A previous study demonstrated importance of Prx1 in the initiation of pulmonary inflammation following exposure to non-lethal levels of ozone [29].…”

Close teamwork between Nrf2 and peroxiredoxins 1 and 6 for the regulation of prostaglandin D2 and E2 production in macrophages in acute inflammation

Protein Moonlighting and Human Health and Idiopathic Human Disease

The functional role of soluble proteins acquired by extracellular vesicles