Abstract

The cGAS–STING signalling pathway has emerged as a key mediator of inflammation in the settings of infection, cellular stress and tissue damage. Underlying this broad involvement of the cGAS–STING pathway is its capacity to sense and regulate the cellular response towards microbial and host-derived DNAs, which serve as ubiquitous danger-associated molecules. Insights into the structural and molecular biology of the cGAS–STING pathway have enabled the development of selective small-molecule inhibitors with the potential to target the cGAS–STING axis in a number of inflammatory diseases in humans. Here, we outline the principal elements of the cGAS–STING signalling cascade and discuss the general mechanisms underlying the association of cGAS–STING activity with various autoinflammatory, autoimmune and degenerative diseases. Finally, we outline the chemical nature of recently developed cGAS and STING antagonists and summarize their potential clinical applications. The cGAS–STING pathway drives innate immune activation in response to cytosolic DNA. This is important for immunity to bacteria and viruses, but aberrant cGAS–STING activity is also linked to inflammatory disease. Here, Ablasser and colleagues discuss how cGAS–STING signalling contributes to various autoimmune, inflammatory and degenerative diseases and describe the novel therapeutics targeting this pathway.

Keywords

StingInnate immune systemInflammationStimulator of interferon genesBiologySignal transductionMediatorImmune systemCell biologyImmunology

MeSH Terms

Adaptor ProteinsSignal TransducingAnimalsAutophagyCell DeathCell ProliferationDNAMitochondrialEnzyme InhibitorsGain of Function MutationHumansInflammationInflammation MediatorsMembrane ProteinsModelsBiologicalModelsMolecularNucleotidesCyclicNucleotidyltransferasesSignal Transduction

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Publication Info

Year
2021
Type
review
Volume
21
Issue
9
Pages
548-569
Citations
1862
Access
Closed

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Cite This

Alexiane Decout, Jason D. Katz, Shankar Venkatraman et al. (2021). The cGAS–STING pathway as a therapeutic target in inflammatory diseases. Nature reviews. Immunology , 21 (9) , 548-569. https://doi.org/10.1038/s41577-021-00524-z

Identifiers

DOI
10.1038/s41577-021-00524-z
PMID
33833439
PMCID
PMC8029610

Data Quality

Data completeness: 86%