AI Article Synopsis

  • CRISPR-Cas systems are bacterial defenses that help combat viruses and genetic elements, but little is known about their evolution in new environments.* -
  • In a study of a poultry pathogen that shifted to a passerine host 30 years ago, researchers observed changes in CRISPR-Cas components, showing adaptations to new viral pressures.* -
  • Over time, isolates exhibited a rise in non-functional CRISPR-Cas systems, coinciding with the passerine host's resistance evolution, indicating that this inactivation may have been crucial for bacterial adaptation and increased virulence.*

Article Abstract

Clustered regularly interspaced short palindromic repeat (CRISPR)-Cas systems are bacterial defences that target bacteriophages and mobile genetic elements. How these defences evolve in novel host environments remains largely unknown. We studied the evolution of the CRISPR-Cas system in (also named ), a bacterial pathogen of poultry that jumped into a passerine host ~30 years ago. Over the decade following the host shift, all isolates displaying a functional CRISPR-Cas system were found not only to harbour completely new sets of spacers, but the DNA protospacer adjacent motif recognized by the main effector Cas9 (MgCas9) was also different. These changes in CRISPR-Cas diversity and specificity are consistent with a change in the community of phages and mobile elements infecting as it colonized the novel host. In the years following the host shift, we also detected a gradual rise in isolates displaying non-functional MgCas9. After 12 years, all circulating isolates harboured inactive forms only. This loss of CRISPR-Cas function comes at a time when the passerine host is known to have evolved widespread resistance, which in turn drove the evolution of increasing virulence through antagonistic coevolution. Such striking concordance in the rise of inactivated forms of CRISPR-Cas and the evolution of host resistance suggests that the inactivation of the CRISPR-Cas system was necessary for enabling adaptive bacterial responses to host-driven selection. We highlight the need to consider both host and pathogen selection pressures on bacteria for understanding the evolution of CRISPR-Cas systems and the key factors driving the emergence of a pathogenic bacterium in a novel host.

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Source
http://dx.doi.org/10.1099/mgen.0.001320DOI Listing

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