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OPTN recruitment to a Golgi-proximal compartment regulates immune signalling and cytokine secretion

Thomas O’loughlin, Antonina J. Kruppa, André Luís Ribeiro Ribeiro, James R. Edgar, Abdulaziz Ghannam, Andrew Smith, Folma Buß

2020Journal of Cell Science37 citationsDOIOpen Access PDF

Abstract

mutations are associated with several human diseases. Here, we show that, in response to viral RNA, OPTN translocates to foci in the perinuclear region, where it negatively regulates NF-κB and IRF3 signalling pathways and downstream pro-inflammatory cytokine secretion. These OPTN foci consist of a tight cluster of small membrane vesicles, which are positive for ATG9A. Disease mutations in OPTN linked to primary open-angle glaucoma (POAG) cause aberrant foci formation in the absence of stimuli, which correlates with the ability of OPTN to inhibit signalling. By using proximity labelling proteomics, we identify the linear ubiquitin assembly complex (LUBAC), CYLD and TBK1 as part of the OPTN interactome and show that these proteins are recruited to this OPTN-positive perinuclear compartment. Our work uncovers a crucial role for OPTN in dampening NF-κB and IRF3 signalling through the sequestration of LUBAC and other positive regulators in this viral RNA-induced compartment, leading to altered pro-inflammatory cytokine secretion.

Topics & Concepts

BiologySecretionGolgi apparatusCompartment (ship)SignallingCell biologyImmune systemCytokineSecretory pathwayImmunologyBiochemistryEndoplasmic reticulumGeologyOceanographyInflammasome and immune disordersinterferon and immune responsesEndoplasmic Reticulum Stress and Disease
OPTN recruitment to a Golgi-proximal compartment regulates immune signalling and cytokine secretion | Litcius