Publication | Closed Access
Recycling endosome-dependent and -independent mechanisms for IL-10 secretion in LPS-activated macrophages
54
Citations
28
References
2012
Year
ImmunologyImmune RegulationLps-activated MacrophagesImmunologic MechanismInnate ImmunityInflammationAutophagyIl-10 SecretionSecretory PathwayCell SignalingAutoimmune DiseaseCell TraffickingAutoimmunityCell BiologyPhagocyteCytokineSignal TransductionActivated MacrophagesExcessive Inflammatory ResponsesTrafficking PathwaysIntracellular Trafficking-Independent MechanismsMedicine
IL-10 is a key anti-inflammatory cytokine secreted by activated macrophages as a feedback control mechanism to prevent excessive inflammatory responses. Here, we define multiple intracellular trafficking pathways involved in the secretion of newly synthesized IL-10 from macrophages following TLR4 activation with LPS, and show how this relates to the previously defined trafficking pathways for IL-6 and TNF in macrophages simultaneously producing these proinflammatory cytokines. IL-10 exits the Golgi in multiple tubular carriers, including those dependent on p230GRIP. Some of the IL-10 is then delivered to recycling endosomes, where cytokine sorting may occur prior to its release. Another portion of the IL-10 is delivered to the cell surface in distinct vesicles colabeled for apoE. Thus, we show at least two post-Golgi pathways via which IL-10 is trafficked, ensuring its secretion from activated macrophages under different physiological conditions.
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