Attenuation of cGAS/STING activity during mitosis.
Brittany L UhlornEduardo R GamezShuaizhi LiSamuel K CamposPublished in: Life science alliance (2020)
The innate immune system recognizes cytosolic DNA associated with microbial infections and cellular stress via the cGAS/STING pathway, leading to activation of phospho-IRF3 and downstream IFN-I and senescence responses. To prevent hyperactivation, cGAS/STING is presumed to be nonresponsive to chromosomal self-DNA during open mitosis, although specific regulatory mechanisms are lacking. Given a role for the Golgi in STING activation, we investigated the state of the cGAS/STING pathway in interphase cells with artificially vesiculated Golgi and in cells arrested in mitosis. We find that whereas cGAS activity is impaired through interaction with mitotic chromosomes, Golgi integrity has little effect on the enzyme's production of cGAMP. In contrast, STING activation in response to either foreign DNA (cGAS-dependent) or exogenous cGAMP is impaired by a vesiculated Golgi. Overall, our data suggest a secondary means for cells to limit potentially harmful cGAS/STING responses during open mitosis via natural Golgi vesiculation.
Keyphrases
- induced apoptosis
- cell cycle arrest
- immune response
- endoplasmic reticulum
- cell free
- minimally invasive
- dendritic cells
- cell death
- magnetic resonance imaging
- transcription factor
- signaling pathway
- stress induced
- endothelial cells
- deep learning
- dna methylation
- computed tomography
- mass spectrometry
- cell proliferation
- pi k akt
- data analysis
- atomic force microscopy