AI Article Synopsis

  • Temperate bacteriophages can follow two paths after infecting a bacteria: the lysogenic cycle or the lytic cycle.
  • The choice depends on specific proteins in the virus that control its actions, particularly a protein called CI and another called MOR that influences it.
  • Researchers discovered how MOR works by studying its structure and found that if MOR doesn’t work correctly, the virus can’t choose the lytic cycle, which is important for its life cycle and is similar in other related viruses.

Article Abstract

Temperate bacteriophages can enter one of two life cycles following infection of a sensitive host: the lysogenic or the lytic life cycle. The choice between the two alternative life cycles is dependent upon a tight regulation of promoters and their cognate regulatory proteins within the phage genome. We investigated the genetic switch of TP901-1, a bacteriophage of , controlled by the CI repressor and the modulator of repression (MOR) antirepressor and their interactions with DNA. We determined the solution structure of MOR, and we solved the crystal structure of MOR in complex with the N-terminal domain of CI, revealing the structural basis of MOR inhibition of CI binding to the DNA operator sites. N NMR Carr-Purcell-Meiboom-Gill (CPMG) relaxation dispersion and rotating frame measurements demonstrate that MOR displays molecular recognition dynamics on two different time scales involving a repacking of aromatic residues at the interface with CI. Mutations in the CI:MOR binding interface impair complex formation in vitro, and when introduced in vivo, the bacteriophage switch is unable to choose the lytic life cycle showing that the CI:MOR complex is essential for proper functioning of the genetic switch. On the basis of sequence alignments, we show that the structural features of the MOR:CI complex are likely conserved among a larger family of bacteriophages from human pathogens implicated in transfer of antibiotic resistance.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7456139PMC
http://dx.doi.org/10.1073/pnas.2005218117DOI Listing

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