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Sequence-Specific Targeting of Bacterial Resistance Genes Increases Antibiotic Efficacy
Author(s) -
Dilay Hazal Ayhan,
Yusuf Talha Tamer,
Mohammed Ali Akbar,
Stacey M. Bailey,
Michael Wong,
Seth M. Daly,
David E. Greenberg,
Erdal Toprak
Publication year - 2016
Publication title -
plos biology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 4.127
H-Index - 271
eISSN - 1545-7885
pISSN - 1544-9173
DOI - 10.1371/journal.pbio.1002552
Subject(s) - antibiotics , biology , bacteria , escherichia coli , oligomer , antibiotic resistance , microbiology and biotechnology , efflux , pathogenic bacteria , gene , enterobacteriaceae , genetics , chemistry , organic chemistry
The lack of effective and well-tolerated therapies against antibiotic-resistant bacteria is a global public health problem leading to prolonged treatment and increased mortality. To improve the efficacy of existing antibiotic compounds, we introduce a new method for strategically inducing antibiotic hypersensitivity in pathogenic bacteria. Following the systematic verification that the AcrAB-TolC efflux system is one of the major determinants of the intrinsic antibiotic resistance levels in Escherichia coli , we have developed a short antisense oligomer designed to inhibit the expression of acrA and increase antibiotic susceptibility in E . coli . By employing this strategy, we can inhibit E . coli growth using 2- to 40-fold lower antibiotic doses, depending on the antibiotic compound utilized. The sensitizing effect of the antisense oligomer is highly specific to the targeted gene’s sequence, which is conserved in several bacterial genera, and the oligomer does not have any detectable toxicity against human cells. Finally, we demonstrate that antisense oligomers improve the efficacy of antibiotic combinations, allowing the combined use of even antagonistic antibiotic pairs that are typically not favored due to their reduced activities.

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