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Article Dans Une Revue The International Society of Microbiologial Ecology Journal Année : 2024

Escherichia coli CRISPR arrays from early life fecal samples preferentially target prophages

Résumé

Abstract CRISPR-Cas systems are defense mechanisms against phages and other nucleic acids that invade bacteria and archaea. In Escherichia coli, it is generally accepted that CRISPR-Cas systems are inactive in laboratory conditions due to a transcriptional repressor. In natural isolates, it has been shown that CRISPR arrays remain stable over the years and that most spacer targets (protospacers) remain unknown. Here, we re-examine CRISPR arrays in natural E. coli isolates and investigate viral and bacterial genomes for spacer targets using a bioinformatics approach coupled to a unique biological dataset. We first sequenced the CRISPR1 array of 1769 E. coli isolates from the fecal samples of 639 children obtained during their first year of life. We built a network with edges between isolates that reflect the number of shared spacers. The isolates grouped into 34 modules. A search for matching spacers in bacterial genomes showed that E. coli spacers almost exclusively target prophages. While we found instances of self-targeting spacers, those involving a prophage and a spacer within the same bacterial genome were rare. The extensive search for matching spacers also expanded the library of known E. coli protospacers to 60%. Altogether, these results suggest that E. coli’s CRISPR-Cas is an anti-prophage system and highlight the importance of reconsidering the criteria use to deem CRISPR-Cas systems active.

Dates et versions

hal-04662284 , version 1 (25-07-2024)

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Citer

Moïra Dion, Shiraz Shah, Ling Deng, Jonathan Thorsen, Jakob Stokholm, et al.. Escherichia coli CRISPR arrays from early life fecal samples preferentially target prophages. The International Society of Microbiologial Ecology Journal, 2024, 18 (1), pp.986-998. ⟨10.1093/ismejo/wrae005⟩. ⟨hal-04662284⟩
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