Genome-wide analysis captures the determinants of the antibiotic cross-resistance interaction network

Lázár, Viktória; Nagy, István; Spohn, Réka; Csörgő, Bálint; Györkei, Ádám; Nyerges, Ákos; Horváth, Balázs; Vörös, Andrea; Busa-Fekete, Róbert; Hrtyan, Mónika; Bogos, Balázs; Méhi, Orsolya; Fekete, G.; Szappanos, Balázs; Kégl, Balázs; Papp, Balázs; Pál, Csaba

doi:10.1038/ncomms5352

Cited by 215 publications

(287 citation statements)

References 57 publications

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“…Experimental evolution studies of evolution of antibiotic resistance showed that in many cases resistance-conferring mutations arose both in target and off-pathway genes (5,11). However, mutations conferring resistance against trimethoprim (TMP) were largely limited to the target gene, namely the ORF and upstream region of folA, the gene encoding dihydrofolate reductase (DHFR) (1,5,11).…”

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confidence: 99%

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Biophysical principles predict fitness landscapes of drug resistance

Rodrigues

Bershtein

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

156

265

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Fitness landscapes of drug resistance constitute powerful tools to elucidate mutational pathways of antibiotic escape. Here, we developed a predictive biophysics-based fitness landscape of trimethoprim (TMP) resistance for Escherichia coli dihydrofolate reductase (DHFR). We investigated the activity, binding, folding stability, and intracellular abundance for a complete set of combinatorial DHFR mutants made out of three key resistance mutations and extended this analysis to DHFR originated from Chlamydia muridarum and Listeria grayi. We found that the acquisition of TMP resistance via decreased drug affinity is limited by a trade-off in catalytic efficiency. Protein stability is concurrently affected by the resistant mutants, which precludes a precise description of fitness from a single molecular trait. Application of the kinetic flux theory provided an accurate model to predict resistance phenotypes (IC50) quantitatively from a unique combination of the in vitro protein molecular properties. Further, we found that a controlled modulation of the GroEL/ES chaperonins and Lon protease levels affects the intracellular steady-state concentration of DHFR in a mutation-specific manner, whereas IC50 is changed proportionally, as indeed predicted by the model. This unveils a molecular rationale for the pleiotropic role of the protein quality control machinery on the evolution of antibiotic resistance, which, as we illustrate here, may drastically confound the evolutionary outcome. These results provide a comprehensive quantitative genotype–phenotype map for the essential enzyme that serves as an important target of antibiotic and anticancer therapies.

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confidence: 99%

“…However, mutations conferring resistance against trimethoprim (TMP) were largely limited to the target gene, namely the ORF and upstream region of folA, the gene encoding dihydrofolate reductase (DHFR) (1,5,11). DHFR is an essential core metabolic enzyme that converts dihydrofolate to tetrahydrofolate-a main source of carbon atoms in several key pathways.…”

mentioning

confidence: 99%

Biophysical principles predict fitness landscapes of drug resistance

Rodrigues

Bershtein

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

156

265

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“…Indeed, most pathogenic bacteria become resistant with time to the action of antibiotics. 2,3 This effect represents a paramount medical problem so that new molecules and compounds with high and persistent antibacterial activity are required to face the challenge of emerging infections and the global spread of drug-resistant microbial pathogens. 4 In addition to the treatment of infections, novel preservatives are essential in pharmaceutical and cosmetic areas as an alternative solution to the widely used esters of p-hydroxybenzoic acid (parabens).…”

Section: Introductionmentioning

confidence: 99%

Negatively charged silver nanoparticles with potent antibacterial activity and reduced toxicity for pharmaceutical preparations

Salvioni¹,

Galbiati²,

Collico³

et al. 2017

IJN

122

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“…The acquisition of antibiotic resistance under optimized culture conditions and the underlying molecular mechanisms causing the cellular response are well documented (2,(10)(11)(12). The second aim of this study was to investigate whether additional stress factors, such as low pH or increased NaCl concentrations, influence the ability of the cell to acquire antibiotic resistance de novo.…”

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confidence: 99%

Effects of Stress, Reactive Oxygen Species, and the SOS Response on De Novo Acquisition of Antibiotic Resistance in Escherichia coli

Händel

Hoeksema

Mata

et al. 2016

Antimicrob Agents Chemother

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. In this study, the contribution of several individual genes to the de novo acquisition of antibiotic resistance in Escherichia coli was investigated using mutants with deletions of genes known to be involved in antibiotic resistance. The results indicate that recA, vital for the SOS response, plays a crucial role in the development of antibiotic resistance. Likewise, deletion of global transcriptional regulators, such as gadE or soxS, involved in pH homeostasis and superoxide removal, respectively, can slow the acquisition of resistance to a degree depending on the antibiotic. Deletion of the transcriptional regulator soxS, involved in superoxide removal, slowed the acquisition of resistance to enrofloxacin. Acquisition of resistance occurred at a lower rate in the presence of a second stress factor, such as a lowered pH or increased salt concentration, than in the presence of optimal growth conditions. The overall outcome suggests that a central cellular mechanism is crucial for the development of resistance and that genes involved in the regulation of transcription play an essential role. The actual cellular response, however, depends on the class of antibiotic in combination with environmental conditions. A ntibiotic-resistant bacteria pose a serious threat to human health, as the costs of therapy of infections caused by such bacteria increase and the treatment outcome is negatively affected. Bacteria can become resistant de novo by genetic or phenotypic changes and also through the acquisition of resistance-conferring mobile genetic elements. Resistance to antibiotics is rapidly induced as a result of exposure to stepwise increasing sublethal drug concentrations (1). In less than 100 generations, bacterial cells developed genetic mutations and permanent transcriptional changes (2). On the one hand, these cellular modifications allow the population to grow in the presence of high antibiotic concentrations, but on the other hand, they may decrease fitness or cause a metabolic burden (1-3). This metabolic cost does not necessarily come in the form of an increased energy requirement. For example, the adaptation of Escherichia coli to amoxicillin was accompanied by a reduced ecological range, because resistant cells were less able to grow well under adverse external conditions (4).In order to devise measures to prevent or at least slow the development of antibiotic resistance, it is essential to understand the reaction of bacteria to drug exposure at the molecular level. Genes that were permanently differentially regulated in E. coli cells made resistant to amoxicillin, enrofloxacin, or tetracycline compared to their regulation in their sensitive ancestor (2) are likely to play a role in the development of resistance. For example, gadABC and hdeA, which confer resistance to acidic conditions, were differentially expressed in cells made permanently resistant to amoxicillin, enrofloxacin, or tetracycline by exposure to stepwise increasing antibiotic levels. The change in the expression of gadABC and hdeA was the ...

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Genome-wide analysis captures the determinants of the antibiotic cross-resistance interaction network

Cited by 215 publications

References 57 publications

Biophysical principles predict fitness landscapes of drug resistance

Biophysical principles predict fitness landscapes of drug resistance

Negatively charged silver nanoparticles with potent antibacterial activity and reduced toxicity for pharmaceutical preparations

Effects of Stress, Reactive Oxygen Species, and the SOS Response on De Novo Acquisition of Antibiotic Resistance in Escherichia coli

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