IL-23R (human) (rec.) (His)

AdipoGen Life Sciences

IL-23R (human) (rec.) (His)

10

Research Use Only

1 mg/ml

>95%

IL23R

interleukin 23 receptor

PSORS7, interleukin-23 receptor, IL-23 receptor

Interleukin-23 receptor

IL-23 is a heterodimeric cytokine containing two subunits: p19 (encoded by IL23A) and p40 (encoded by IL12B). IL-23 signals via a heterodimeric receptor, IL-23R, composed of a specific subunit, IL23R, and the IL12Rbeta1 subunit, which is shared with the IL-12 receptor. IL-23R promotes mainly STAT3, but also STAT1, STAT4 and STAT5 phosphorylation. IL-23 supports the expansion and survival of established murine Th17 cells and enhances IFN-gamma production by memory CD4+ T cells. IL-23R is expressed on T cells, B cells, myeloid cells and NK cells. IL-23 signaling pathway is important in the pathogenesis of several chronic inflammatory diseases, including axial spondyloarthritis, axial spondyloarthritis, Crohns disease and psoriasis. Cellular senescence is an age-associated mechanism that contributes to pathogenesis in diverse organ systems. In a recent study, it was observed that IL-23R, CCL5 and other proteins show age-dependent increases in circulation and are critical aging biomarkers, linked to senescence and are reduced by senotherapeutic agents. In human plasma, IL-23R abundance increases with age in both women and men. So, IL-23R seems to be a mediators of interorgan signaling mediated by senescent cells. - Recombinant Protein. Extracellular domain of human IL-23R (aa 24-354) is fused at the C-terminus to a His-tag Lyophilized. Contains PBS. IL-23 is a heterodimeric cytokine containing two subunits: p19 (encoded by IL23A) and p40 (encoded by IL12B). IL-23 signals via a heterodimeric receptor, IL-23R, composed of a specific subunit, IL23R, and the IL12Rbeta1 subunit, which is shared with the IL-12 receptor. IL-23R promotes mainly STAT3, but also STAT1, STAT4 and STAT5 phosphorylation. IL-23 supports the expansion and survival of established murine Th17 cells and enhances IFN-gamma production by memory CD4+ T cells. IL-23R is expressed on T cells, B cells, myeloid cells and NK cells. IL-23 signaling pathway is important in the pathogenesis of several chronic inflammatory diseases, including axial spondyloarthritis, axial spondyloarthritis, Crohns disease and psoriasis. Cellular senescence is an age-associated mechanism that contributes to pathogenesis in diverse organ systems. In a recent study, it was observed that IL-23R, CCL5 and other proteins show age-dependent increases in circulation and are critical aging biomarkers, linked to senescence and are reduced by senotherapeutic agents. In human plasma, IL-23R abundance increases with age in both women and men. So, IL-23R seems to be a mediators of interorgan signaling mediated by senescent cells.

-20°C,2°C to 8°C

41116120

Human