4.8 Article

Genome manipulation by guide-directed Argonaute cleavage

Journal

NUCLEIC ACIDS RESEARCH
Volume 51, Issue 8, Pages 4078-4085

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/nar/gkad188

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A recent study shows that CbAgo, a prokaryotic argonaute, can induce DNA interference and generate double-stranded breaks in target DNAs. The study demonstrates that CbAgo can cleave genome target sites and induce chromosome recombination in Escherichia coli. The findings suggest that the guide-directed cleavage of pAgo on the host genome is mutagenic and can be utilized in genetic manipulation.
Many prokaryotic argonautes (pAgos) mediate DNA interference by using small DNA guides to cleave target DNA. A recent study shows that CbAgo, a pAgo from Clostridium butyricum, induces DNA interference between homologous sequences and generates double-stranded breaks (DSBs) in target DNAs. This mechanism enables the host to defend against invading DNAs such as plasmids and viruses. However, whether such a CbAgo-mediated DNA cleavage is mutagenic remains unexplored. Here we demonstrate that CbAgo, directed by plasmid-encoded guide sequences, can cleave genome target sites and induce chromosome recombination between downstream homologous sequences in Escherichia coli. The recombination rate correlates well with pAgo DNA cleavage activity and the mechanistic study suggests the recombination involves DSBs and RecBCD processing. In RecA-deficient E. coli strain, guide-directed CbAgo cleavage on chromosomes severely impairs cell growth, which can be utilized as counter-selection to assist Lambda-Red recombineering. These findings demonstrate the guide-directed cleavage of pAgo on the host genome is mutagenic and can lead to different outcomes according to the function of the host DNA repair machinery. We anticipate this novel DNA-guided interference to be useful in broader genetic manipulation. Our study also provides an in vivo assay to characterize or engineer pAgo DNA cleavage activity.

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