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Items: 3

1.

Targeting bacterial gyrase with cystobactamid, fluoroquinolone and aminocoumarin antibiotics induces distinct molecular signatures in Pseudomonas aeruginosa

(Submitter supplied) The design of novel antibiotics that break antimicrobial resistance relies on a profound understanding of their mechanism of action. While it has been shown that the cellular effects of antibiotics cluster according to their molecular targets, we investigated whether compounds binding to different sites of the same target can be differentiated by their transcriptome or metabolome signatures. The effects of three fluoroquinolones, two aminocoumarins and two cystobactamids, all inhibiting bacterial gyrase, on Pseudomonas aeruginosa at sub-inhibitory concentrations were captured by RNA sequencing.
Organism:
Pseudomonas aeruginosa UCBPP-PA14
Type:
Expression profiling by high throughput sequencing
Platform:
GPL27892
24 Samples
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Series
Accession:
GSE166602
ID:
200166602
2.

Illumina NovaSeq 6000 (Pseudomonas aeruginosa UCBPP-PA14)

Organism:
Pseudomonas aeruginosa UCBPP-PA14
9 Series
1215 Samples
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Platform
Accession:
GPL27892
ID:
100027892
3.

AR351_1

Organism:
Pseudomonas aeruginosa UCBPP-PA14
Source name:
RNASeq of planctonic culture of P. aeruginosa UCBPP-PA14 treated with IC50 of cystobactamid AR351 from OD 0.05 to OD 0.6
Platform:
GPL27892
Series:
GSE166602
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Sample
Accession:
GSM5076113
ID:
305076113
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db=gds|term=GSM5076113[Accession]|query=1|qty=2|blobid=MCID_674c4b3896d9ad04062460b5|ismultiple=true|min_list=5|max_list=20|def_tree=20|def_list=|def_view=|url=/Taxonomy/backend/subset.cgi?|trace_url=/stat?
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