Interleukin-6 secretion is limited by self-signaling in endosomesVerboogen, D. R. J., Revelo, N. H., Ter Beest, M. & van den Bogaart, G., Feb-2019, In : The Journal of Cell Biology. 11, 2, p. 144-157 14 p.
Research output: Contribution to journal › Article › Academic › peer-review
Cells producing cytokines often express the receptor for the same cytokine, which makes them prone to autocrine signaling. How cytokine release and signaling are regulated in the same cell is not understood. In this study, we demonstrate that signaling by exogenous and self-synthesized inflammatory cytokine interleukin-6 (IL-6) within endosomal compartments acts as a cellular brake that limits synthesis of IL-6. Our data show that IL-6 is internalized by dendritic cells and signals from endosomal compartments containing the IL-6 receptor. Newly synthesized IL-6 also traffics via these endosomal compartments and signals in transit to the plasma membrane. This allows activation of STAT3 which in turn limits Toll-like receptor 4 stimulant lipopolysaccharide (LPS) triggered transcription of IL-6. Long-term exposure to LPS removes this brake via inhibition of STAT3 by increased expression of suppressor of cytokine signaling 3 (SOCS3) and results in fully-fledged IL-6 production. This transient regulation could prevent excessive IL-6 production during early infections.
|Number of pages||14|
|Journal||The Journal of Cell Biology|
|Early online date||16-Jul-2018|
|Publication status||Published - Feb-2019|
- membrane traffickin, cytokine release, exocytosis, interleukin-6, endosomal signaling, PRO-INFLAMMATORY CYTOKINES, BLOOD MONONUCLEAR-CELLS, DENDRITIC CELLS, RECEPTOR-ALPHA, HUMAN IL-6, MAXIMAL ACTIVATION, IN-VIVO, STAT3, SERUM, GP130