Genome-wide Dynamics of a Bacterial Response to Antibiotics That Target the Cell Envelope

Overview

Journal BMC Genomics

Publisher Biomed Central

Specialty Genetics

Date 2011 May 17

PMID 21569315

Citations 37

Authors

Andy Hesketh

Chris Hill

Jehan Mokhtar

Gabriela Novotna

Ngat Tran

Mervyn Bibb

Hee-Jeon Hong

Affiliations

Soon will be listed here.

Abstract

Background: A decline in the discovery of new antibacterial drugs, coupled with a persistent rise in the occurrence of drug-resistant bacteria, has highlighted antibiotics as a diminishing resource. The future development of new drugs with novel antibacterial activities requires a detailed understanding of adaptive responses to existing compounds. This study uses Streptomyces coelicolor A3(2) as a model system to determine the genome-wide transcriptional response following exposure to three antibiotics (vancomycin, moenomycin A and bacitracin) that target distinct stages of cell wall biosynthesis.

Results: A generalised response to all three antibiotics was identified which involves activation of transcription of the cell envelope stress sigma factor σ(E), together with elements of the stringent response, and of the heat, osmotic and oxidative stress regulons. Attenuation of this system by deletion of genes encoding the osmotic stress sigma factor σ(B) or the ppGpp synthetase RelA reduced resistance to both vancomycin and bacitracin. Many antibiotic-specific transcriptional changes were identified, representing cellular processes potentially important for tolerance to each antibiotic. Sensitivity studies using mutants constructed on the basis of the transcriptome profiling confirmed a role for several such genes in antibiotic resistance, validating the usefulness of the approach.

Conclusions: Antibiotic inhibition of bacterial cell wall biosynthesis induces both common and compound-specific transcriptional responses. Both can be exploited to increase antibiotic susceptibility. Regulatory networks known to govern responses to environmental and nutritional stresses are also at the core of the common antibiotic response, and likely help cells survive until any specific resistance mechanisms are fully functional.

Citing Articles

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Transcriptionally induced nucleoid-associated protein-like in combined-culture serves as a global effector of secondary metabolism.

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σ of Streptomyces coelicolor can function both as a direct activator or repressor of transcription.

Pospisil J, Schwarz M, Zikova A, Vitovska D, Hradilova M, Kolar M Commun Biol. 2024; 7(1):46.

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