Author
Listed:
- Dalton V. Banh
(The Rockefeller University
Weill Cornell/Rockefeller/Sloan Kettering Tri-Institutional MD-PhD Program)
- Cameron G. Roberts
(The Rockefeller University)
- Adrian Morales-Amador
(The Rockefeller University)
- Brandon A. Berryhill
(Department of Biology, Emory University)
- Waqas Chaudhry
(Department of Biology, Emory University)
- Bruce R. Levin
(Department of Biology, Emory University)
- Sean F. Brady
(The Rockefeller University)
- Luciano A. Marraffini
(The Rockefeller University
The Rockefeller University)
Abstract
Cyclic oligonucleotide-based antiphage signalling systems (CBASS) protect prokaryotes from viral (phage) attack through the production of cyclic oligonucleotides, which activate effector proteins that trigger the death of the infected host1,2. How bacterial cyclases recognize phage infection is not known. Here we show that staphylococcal phages produce a structured RNA transcribed from the terminase subunit genes, termed CBASS-activating bacteriophage RNA (cabRNA), which binds to a positively charged surface of the CdnE03 cyclase and promotes the synthesis of the cyclic dinucleotide cGAMP to activate the CBASS immune response. Phages that escape the CBASS defence harbour mutations that lead to the generation of a longer form of the cabRNA that cannot activate CdnE03. Since mammalian oligoadenylate synthetases also bind viral double-stranded RNA during the interferon response, our results reveal a conserved mechanism for the activation of innate antiviral defence pathways.
Suggested Citation
Dalton V. Banh & Cameron G. Roberts & Adrian Morales-Amador & Brandon A. Berryhill & Waqas Chaudhry & Bruce R. Levin & Sean F. Brady & Luciano A. Marraffini, 2023.
"Bacterial cGAS senses a viral RNA to initiate immunity,"
Nature, Nature, vol. 623(7989), pages 1001-1008, November.
Handle:
RePEc:nat:nature:v:623:y:2023:i:7989:d:10.1038_s41586-023-06743-9
DOI: 10.1038/s41586-023-06743-9
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