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Bacteriostatic antibiotics promote the evolution of CRISPR-Cas immunity
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AbstractPhage therapy can be used in combination with antibiotics to combat infections with bacterial pathogens1–3. However, bacteria can rapidly evolve phage resistance via receptor mutation, or using their CRISPR-Cas adaptive immune systems4, which insert short phage-derived sequences into CRISPR loci in the bacterial genome5to guide sequence-specific cleavage of cognate sequences6. Unlike CRISPR-Cas immunity, mutation of the phage receptor leads to attenuated virulence when the opportunistic pathogenPseudomonas aeruginosais infected with its phage DMS3vir7, which underscores the need to predict how phage resistance evolves under clinically relevant conditions. Here, using eight antibiotics with various modes of action, we show that bacteriostatic antibiotics (which inhibit cell growth without killing) specifically promote evolution of CRISPR-Cas immunity inP. aeruginosaby slowing down phage development and providing more time for cells to acquire phage-derived sequences and mount an immune response. Our data show that some antimicrobial treatments can contribute to the evolution of phage-resistant pathogens with high virulence.
Cold Spring Harbor Laboratory
Title: Bacteriostatic antibiotics promote the evolution of CRISPR-Cas immunity
Description:
AbstractPhage therapy can be used in combination with antibiotics to combat infections with bacterial pathogens1–3.
However, bacteria can rapidly evolve phage resistance via receptor mutation, or using their CRISPR-Cas adaptive immune systems4, which insert short phage-derived sequences into CRISPR loci in the bacterial genome5to guide sequence-specific cleavage of cognate sequences6.
Unlike CRISPR-Cas immunity, mutation of the phage receptor leads to attenuated virulence when the opportunistic pathogenPseudomonas aeruginosais infected with its phage DMS3vir7, which underscores the need to predict how phage resistance evolves under clinically relevant conditions.
Here, using eight antibiotics with various modes of action, we show that bacteriostatic antibiotics (which inhibit cell growth without killing) specifically promote evolution of CRISPR-Cas immunity inP.
aeruginosaby slowing down phage development and providing more time for cells to acquire phage-derived sequences and mount an immune response.
Our data show that some antimicrobial treatments can contribute to the evolution of phage-resistant pathogens with high virulence.
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