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A targeted gene-silencing screen finds a blocker of a key bacterial protein that helps build new proteins

Updated

Abstract

CIMPLE enables genomic coverage of antibacterial targets through optimized CRISPR interference.

  • Pooled libraries of essential genes can help characterize the mechanisms of new antibiotics.
  • Uneven growth of mutant strains can lead to the loss of important targets in pooled libraries.
  • CIMPLE was constructed to model and adjust mutant abundance, improving detection of antibacterial targets.
  • Chemical-genetic profiling identified a novel compound that inhibits peptidyl-tRNA hydrolase in bacteria.
  • CIMPLE combines advantages of both arrayed and pooled CRISPR interference libraries for antibiotic discovery.

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