Literature DB >> 25425575

Cytosolic RNA:DNA hybrids activate the cGAS-STING axis.

Arun K Mankan1, Tobias Schmidt1, Dhruv Chauhan1, Marion Goldeck2, Klara Höning1, Moritz Gaidt1, Andrew V Kubarenko1, Liudmila Andreeva3, Karl-Peter Hopfner3, Veit Hornung4.   

Abstract

Intracellular recognition of non-self and also self-nucleic acids can result in the initiation of potent pro-inflammatory and antiviral cytokine responses. Most recently, cGAS was shown to be critical for the recognition of cytoplasmic dsDNA. Binding of dsDNA to cGAS results in the synthesis of cGAMP(2'-5'), which then binds to the endoplasmic reticulum resident protein STING. This initiates a signaling cascade that triggers the induction of an antiviral immune response. While most studies on intracellular nucleic acids have focused on dsRNA or dsDNA, it has remained unexplored whether cytosolic RNA:DNA hybrids are also sensed by the innate immune system. Studying synthetic RNA:DNA hybrids, we indeed observed a strong type I interferon response upon cytosolic delivery of this class of molecule. Studies in THP-1 knockout cells revealed that the recognition of RNA:DNA hybrids is completely attributable to the cGAS-STING pathway. Moreover, in vitro studies showed that recombinant cGAS produced cGAMP upon RNA:DNA hybrid recognition. Altogether, our results introduce RNA:DNA hybrids as a novel class of intracellular PAMP molecules and describe an alternative cGAS ligand next to dsDNA.
© 2014 The Authors.

Entities:  

Keywords:  RNA:DNA hybrids; STING; cGAS; innate immunity; pattern recognition receptor

Mesh:

Substances:

Year:  2014        PMID: 25425575      PMCID: PMC4282641          DOI: 10.15252/embj.201488726

Source DB:  PubMed          Journal:  EMBO J        ISSN: 0261-4189            Impact factor:   11.598


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