Atypical organizations and epistatic interactions of CRISPRs and cas clusters in genomes and their mobile genetic elements

Author:

Bernheim Aude1234ORCID,Bikard David2ORCID,Touchon Marie1,Rocha Eduardo P C1ORCID

Affiliation:

1. Microbial Evolutionary Genomics, Institut Pasteur, CNRS, UMR3525, 25–28 rue Dr. Roux, Paris 75015, France

2. Synthetic Biology Group, Institut Pasteur, 25–28 rue Dr. Roux, Paris 75015, France

3. AgroParisTech, F-75005 Paris, France

4. Ecole doctorale Frontières du vivant, Université Paris Diderot, Université Sorbonne Paris Cité, 75013 Paris, France

Abstract

Abstract Prokaryotes use CRISPR–Cas systems for adaptive immunity, but the reasons for the frequent existence of multiple CRISPRs and cas clusters remain poorly understood. Here, we analysed the joint distribution of CRISPR and cas genes in a large set of fully sequenced bacterial genomes and their mobile genetic elements. Our analysis suggests few negative and many positive epistatic interactions between Cas subtypes. The latter often result in complex genetic organizations, where a locus has a single adaptation module and diverse interference mechanisms that might provide more effective immunity. We typed CRISPRs that could not be unambiguously associated with a cas cluster and found that such complex loci tend to have unique type I repeats in multiple CRISPRs. Many chromosomal CRISPRs lack a neighboring Cas system and they often have repeats compatible with the Cas systems encoded in trans. Phages and 25 000 prophages were almost devoid of CRISPR–Cas systems, whereas 3% of plasmids had CRISPR–Cas systems or isolated CRISPRs. The latter were often compatible with the chromosomal cas clusters, suggesting that plasmids can co-opt the latter. These results highlight the importance of interactions between CRISPRs and cas present in multiple copies and in distinct genomic locations in the function and evolution of bacterial immunity.

Funder

Pasteur Institute

CNRS

European Research Council

Publisher

Oxford University Press (OUP)

Subject

Genetics

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