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Cleavage of viral DNA by restriction endonucleases stimulates the type II CRISPR-Cas immune response.


ABSTRACT: Prokaryotic organisms have developed multiple defense systems against phages; however, little is known about whether and how these interact with each other. Here, we studied the connection between two of the most prominent prokaryotic immune systems: restriction-modification and CRISPR. While both systems employ enzymes that cleave a specific DNA sequence of the invader, CRISPR nucleases are programmed with phage-derived spacer sequences, which are integrated into the CRISPR locus upon infection. We found that restriction endonucleases provide a short-term defense, which is rapidly overcome through methylation of the phage genome. In a small fraction of the cells, however, restriction results in the acquisition of spacer sequences from the cleavage site, which mediates a robust type II-A CRISPR-Cas immune response against the methylated phage. This mechanism is reminiscent of eukaryotic immunity in which the innate response offers a first temporary line of defense and also activates a second and more robust adaptive response.

SUBMITTER: Maguin P 

PROVIDER: S-EPMC8900293 | biostudies-literature | 2022 Mar

REPOSITORIES: biostudies-literature

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Cleavage of viral DNA by restriction endonucleases stimulates the type II CRISPR-Cas immune response.

Maguin Pascal P   Varble Andrew A   Modell Joshua W JW   Marraffini Luciano A LA  

Molecular cell 20220207 5


Prokaryotic organisms have developed multiple defense systems against phages; however, little is known about whether and how these interact with each other. Here, we studied the connection between two of the most prominent prokaryotic immune systems: restriction-modification and CRISPR. While both systems employ enzymes that cleave a specific DNA sequence of the invader, CRISPR nucleases are programmed with phage-derived spacer sequences, which are integrated into the CRISPR locus upon infection  ...[more]

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