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  Rapid inhibition profiling in Bacillus subtilis to identify the mechanism of action of new antimicrobials

Lamsa, A., López-Garrido, J., Quach, D., Riley, E. P., Pogliano, J., & Pogliano, K. (2016). Rapid inhibition profiling in Bacillus subtilis to identify the mechanism of action of new antimicrobials. ACS Chemical Biology, 11(8), 2222-2231. doi:10.1021/acschembio.5b01050.

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Lamsa, Anne, Author
López-Garrido, Javier1, Author           
Quach, Diana, Author
Riley, Eammon P., Author
Pogliano, Joe, Author
Pogliano, Kit, Author
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1External Organizations, ou_persistent22              

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 Abstract: Increasing antimicrobial resistance has become a major public health crisis. New antimicrobials with novel mechanisms of action (MOA) are desperately needed. We previously developed a method, bacterial cytological profiling (BCP), which utilizes fluorescence microscopy to rapidly identify the MOA of antimicrobial compounds. BCP is based upon our discovery that cells treated with antibiotics affecting different metabolic pathways generate different cytological signatures, providing quantitative information that can be used to determine a compound’s MOA. Here, we describe a system, rapid inhibition profiling (RIP), for creating cytological profiles of new antibiotic targets for which there are currently no chemical inhibitors. RIP consists of the fast, inducible degradation of a target protein followed by BCP. We demonstrate that degrading essential proteins in the major metabolic pathways for DNA replication, transcription, fatty acid biosynthesis, and peptidoglycan biogenesis in Bacillus subtilis rapidly produces cytological profiles closely matching that of antimicrobials targeting the same pathways. Additionally, RIP and antibiotics targeting different steps in fatty acid biosynthesis can be differentiated from each other. We utilize RIP and BCP to show that the antibacterial MOA of four nonsteroidal anti-inflammatory antibiotics differs from that proposed based on in vitro data. RIP is a versatile method that will extend our knowledge of phenotypes associated with inactivating essential bacterial enzymes and thereby allow for screening for molecules that inhibit novel essential targets.

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Language(s): eng - English
 Dates: 2016-052016-08
 Publication Status: Issued
 Pages: -
 Publishing info: -
 Table of Contents: -
 Rev. Type: -
 Identifiers: DOI: 10.1021/acschembio.5b01050
 Degree: -

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Title: ACS Chemical Biology
  Abbreviation : ACS Chem. Biol.
Source Genre: Journal
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Publ. Info: Washington, D.C. : American Chemical Society
Pages: - Volume / Issue: 11 (8) Sequence Number: - Start / End Page: 2222 - 2231 Identifier: ISSN: 1554-8929
CoNE: https://pure.mpg.de/cone/journals/resource/1000000000035040