Circulating mitochondrial DNA-triggered autophagy dysfunction via STING underlies sepsis-related acute lung injury.
Qinjie LiuJie WuXufei ZhangXuanheng LiXiuwen WuYun ZhaoJian-An RenPublished in: Cell death & disease (2021)
The STING pathway and its induction of autophagy initiate a potent immune defense response upon the recognition of pathogenic DNA. However, this protective response is minimal, as STING activation worsens organ damage, and abnormal autophagy is observed during progressive sepsis. Whether and how the STING pathway affects autophagic flux during sepsis-induced acute lung injury (sALI) are currently unknown. Here, we demonstrate that the level of circulating mtDNA and degree of STING activation are increased in sALI patients. Furthermore, STING activation was found to play a pivotal role in mtDNA-mediated lung injury by evoking an inflammatory storm and disturbing autophagy. Mechanistically, STING activation interferes with lysosomal acidification in an interferon (IFN)-dependent manner without affecting autophagosome biogenesis or fusion, aggravating sepsis. Induction of autophagy or STING deficiency alleviated lung injury. These findings provide new insights into the role of STING in the regulatory mechanisms behind extrapulmonary sALI.
Keyphrases
- cell death
- mitochondrial dna
- oxidative stress
- endoplasmic reticulum stress
- copy number
- signaling pathway
- intensive care unit
- acute kidney injury
- septic shock
- end stage renal disease
- dendritic cells
- lipopolysaccharide induced
- ejection fraction
- diabetic rats
- chronic kidney disease
- multiple sclerosis
- newly diagnosed
- immune response
- single molecule
- high glucose
- dna methylation
- endothelial cells
- patient reported outcomes
- genome wide