Your search keyword '"Basting, Preston J."' showing total 5 results

1. Experimental Evolution of Escherichia coli K-12 in the Presence of Proton Motive Force (PMF) Uncoupler Carbonyl Cyanide m-Chlorophenylhydrazone Selects for Mutations Affecting PMF-Driven Drug Efflux Pumps.

Author

Griffith, Jessie M., Basting, Preston J., Bischof, Katarina M., Wrona, Erintrude P., Kunka, Karina S., Tancredi, Anna C., Moore, Jeremy P., Hyman, Miriam R. L., and Slonczewski, Joan L.

Subjects

*ESCHERICHIA coli, *HYDRAZONE derivatives, *GENETIC mutation, *BIOLOGICAL evolution, *BACTERIAL cultures, *BENZOATES

Abstract

Experimental evolution of Escherichia coli K-12 with benzoate, a partial uncoupler of the proton motive force (PMF), selects for mutations that decrease antibiotic resistance. We conducted experimental evolution in the presence of carbonyl cyanide m-chlorophenylhydrazone (CCCP), a strong uncoupler. Cultures were serially diluted daily 1:100 in LBK medium containing 20 to 150 μM CCCP buffered at pH 6.5 or at pH 8.0. After 1,000 generations, the populations tolerated up to 150 μM CCCP. Sequenced isolates had mutations in mprA (emrR), which downregulates the EmrABTolC pump that exports CCCP. A mprA::kanR deletion conferred growth at 60 μM CCCP, though not at the higher levels resisted by evolved strains (150 μM). Some mprA mutant strains also had point mutations affecting emrA, but deletion of emrA abolished the CCCP resistance. Thus, CCCP-evolved isolates contained additional adaptations. One isolate lacked emrA or mprA mutations but had mutations in cecR (ybiH), whose product upregulates drug pumps YbhG and YbhFSR, and in gadE, which upregulates the multidrug pump MdtEF. A cecR::kanR deletion conferred partial resistance to CCCP. Other multidrug efflux genes that had mutations included ybhR and acrAB. The acrB isolate was sensitive to the AcrAB substrates chloramphenicol and tetracycline. Other mutant genes in CCCP-evolved strains include rng (RNase G) and cyaA (adenylate cyclase). Overall, experimental evolution revealed a CCCPdependent fitness advantage for mutations increasing CCCP efflux via EmrA and for mutations that may deactivate proton-driven pumps for drugs not present (cecR, gadE, acrAB, and ybhR). These results are consistent with our previous report of drug sensitivity associated with evolved benzoate tolerance. [ABSTRACT FROM AUTHOR]

Published

2019

2. Acid Evolution of Escherichia coli K-12 Eliminates Amino Acid Decarboxylases and Reregulates Catabolism.

Author

He, Amanda, Penix, Stephanie R., Basting, Preston J., Griffith, Jessie M., Creamer, Kaitlin E., Camperchioli, Dominic, Clark, Michelle W., Gonzales, Alexandra S., Chávez Erazo, Jorge Sebastian, George, Nadja S., Bhagwat, Arvind A., and Slonczewski, Joan L.

Subjects

*ESCHERICHIA coli mutation, *NEONATAL Escherichia coli infections, *ENTEROBACTERIACEAE, *DECARBOXYLASES, *NUCLEOTIDE sequencing

Abstract

Acid-adapted strains of Escherichia coli K-12 W3110 were obtained by serial culture in medium buffered at pH 4.6 (M. M. Harden, A. He, K. Creamer, M. W. Clark, I. Hamdallah, K. A. Martinez, R. L. Kresslein, S. P. Bush, and J. L. Slonczewski, Appl Environ Microbiol 81:1932-1941, 2015, https://doi.org/10.1128/AEM.03494-14). Revised genomic analysis of these strains revealed insertion sequence (IS)-driven insertions and deletions that knocked out regulators CadC (acid induction of lysine decarboxylase), GadX (acid induction of glutamate decarboxylase), and FNR (anaerobic regulator). Each acid-evolved strain showed loss of one or more amino acid decarboxylase systems, which normally help neutralize external acid (pH 5 to 6) and increase survival in extreme acid (pH 2). Strains from populations B11, H9, and F11 had an IS5 insertion or IS-mediated deletion in cadC, while population B11 had a point mutation affecting the arginine activator adiY. The cadC and adiY mutants failed to neutralize acid in the presence of exogenous lysine or arginine. In strain B11-1, reversion of an rpoC (RNA polymerase) mutation partly restored arginine-dependent neutralization. All eight strains showed deletion or downregulation of the Gad acid fitness island. Strains with the Gad deletion lost the ability to produce GABA (gamma-aminobutyric acid) and failed to survive extreme acid. Transcriptome sequencing (RNA-seq) of strain B11-1 showed upregulated genes for catabolism of diverse substrates but downregulated acid stress genes (the biofilm regulator ariR, yhiM, and Gad). Other strains showed downregulation of H2 consumption mediated by hydrogenases (hya and hyb) which release acid. Strains F9-2 and F9-3 had a deletion of fnr and showed downregulation of FNR-dependent genes (dmsABC, frdABCD, hybABO, nikABCDE, and nrfAC). Overall, strains that had evolved in buffered acid showed loss or downregulation of systems that neutralize unbuffered acid and showed altered regulation of catabolism. IMPORTANCE Experimental evolution of an enteric bacterium under a narrow buffered range of acid pH leads to loss of genes that enhance fitness above or below the buffered pH range, including loss of enzymes that may raise external pH in the absence of buffer. Prominent modes of evolutionary change involve IS-mediated insertions and deletions that knock out key regulators. Over generations of acid stress, catabolism undergoes reregulation in ways that differ for each evolving strain. [ABSTRACT FROM AUTHOR]

Published

2017

3. Benzoate- and Salicylate-Tolerant Strains of Escherichia coli K-12 Lose Antibiotic Resistance during Laboratory Evolution.

Author

Creamer, Kaitlin E., Ditmars, Frederick S., Basting, Preston J., Kunka, Karina S., Hamdallah, Issam N., Bush, Sean P., Scott, Zachary, Amanda He, Penix, Stephanie R., Gonzales, Alexandra S., Eder, Elizabeth K., Camperchioli, Dominic W., Berndt, Adama, Clark, Michelle W., Rouhier, Kerry A., and Slonczewski, Joan L.

Subjects

*BENZOATES, *SALICYLATES, *ESCHERICHIA coli, *ANTIBIOTICS, *DRUG resistance in bacteria, *ORGANIC acids

Abstract

Escherichia coli K-12 W3110 grows in the presence of membranepermeant organic acids that can depress cytoplasmic pH and accumulate in the cytoplasm. We conducted experimental evolution by daily diluting cultures in increasing concentrations of benzoic acid (up to 20 mM) buffered at external pH 6.5, a pH at which permeant acids concentrate in the cytoplasm. By 2,000 generations, clones isolated from evolving populations showed increasing tolerance to benzoate but were sensitive to chloramphenicol and tetracycline. Sixteen clones grew to stationary phase in 20 mM benzoate, whereas the ancestral strain W3110 peaked and declined. Similar growth occurred in 10 mM salicylate. Benzoate-evolved strains grew like W3110 in the absence of benzoate, in media buffered at pH 4.8, pH 7.0, or pH 9.0, or in 20 mM acetate or sorbate at pH 6.5. Genomes of 16 strains revealed over 100 mutations, including single-nucleotide polymorphisms (SNPs), large deletions, and insertion knockouts. Most strains acquired deletions in the benzoate-induced multiple antibiotic resistance (Mar) regulon or in associated regulators such as rob and cpxA, as well as the multidrug resistance (MDR) efflux pumps emrA, emrY, and mdtA. Strains also lost or downregulated the Gad acid fitness regulon. In 5 mM benzoate or in 2 mM salicylate (2-hydroxybenzoate), most strains showed increased sensitivity to the antibiotics chloramphenicol and tetracycline; some strains were more sensitive than a marA knockout strain. Thus, our benzoate-evolved strains may reveal additional unknown drug resistance components. Benzoate or salicylate selection pressure may cause general loss of MDR genes and regulators. IMPORTANCE Benzoate is a common food preservative, and salicylate is the primary active metabolite of aspirin. In the gut microbiome, genetic adaptation to salicylate may involve loss or downregulation of inducible multidrug resistance systems. This discovery implies that aspirin therapy may modulate the human gut microbiome to favor salicylate tolerance at the expense of drug resistance. Similar aspirin-associated loss of drug resistance might occur in bacterial pathogens found in arterial plaques. [ABSTRACT FROM AUTHOR]

Published

2017

4. Inverted Regulation of Multidrug Efflux Pumps, Acid Resistance and Porins in 1 Benzoate-Evolved Escherichia coli K-12.

Author

Moore, Jeremy P., Haofan Li, Engmann, Morgan L., Bischof, Katarina M., Kunka, Karina S., Harris, Mary E., Tancredi, Anna C., Ditmars, Frederick S., Basting, Preston J., George, Nadja S., Bhagwat, Arvind A., and Slonczewski, Joan L.

Subjects

*SALICYLATES, *AQUAPORINS, *ESCHERICHIA coli

Abstract

Benzoic acid, a partial uncoupler of the proton motive force (PMF), selects for sensitivity to chloramphenicol and tetracycline during experimental evolution of Escherichia coli K-12. Transcriptomes of E. coli isolates evolved with benzoate showed reversal of benzoate-dependent regulation, including downregulation of multi-drug efflux pumps; the Gad acid resistance regulon; the nitrate reductase narHJ; and the acid-consuming hydrogenase Hyd-3. However, the benzoate-evolved strains had increased expression of OmpF and other large-hole porins that admit fermentable substrates and antibiotics. Candidate genes identified from benzoate-evolved strains were tested for their roles in benzoate tolerance and in chloramphenicol sensitivity. Benzoate or salicylate tolerance was increased by deletion of the Gad activator ariR, or of the slp-gadX acid fitness island encoding Gad regulators and the multi-drug pump mdtEF. Benzoate tolerance was also increased by deletion of multi-drug component emrA, RpoS post- transcriptional regulator cspC, adenosine deaminase add, hydrogenase hyc (Hyd-3), and the RNA chaperone/DNA-binding regulator hfq. Chloramphenicol resistance was decreased by mutations in global regulators, such as RNA polymerase alpha-subunit rpoA, Mar activator rob, and hfq. Deletion of lipopolysaccharide biosynthetic kinase rfaY decreased the rate of growth in chloramphenicol. Isolates from experimental evolution with benzoate had many mutations affecting aromatic biosynthesis and catabolism such as aroF (tyrosine biosynthesis) and apt adenine phosphoribosyltransferase). Overall, benzoate or salicylate exposure selects for loss of multi-drug efflux pumps and of hydrogenases that generate a futile cycle of PMF; and upregulates porins that admit fermentable nutrients and antibiotics. IMPORTANCE Benzoic acid is a common food preservative, and salicylic acid (2-hydroxybenzoic acid) is the active form of aspirin. At high concentration, benzoic acid conducts a proton across the membrane, depleting the proton motive force. In the absence of antibiotics, benzoate exposure selects against proton-driven multidrug efflux pumps and upregulates porins that admit fermentable substrates but also allow entry of antibiotics. Thus, evolution with benzoate, and related molecules such as salicylates, requires a tradeoff for antibiotic sensitivity--a tradeoff that could help define a stable gut microbiome. Benzoate and salicylate are naturally occurring plant signal molecules that may modulate the microbiomes of plants and animal digestive tracts so as to favor fermenters and exclude drug-resistant pathogens. [ABSTRACT FROM AUTHOR]

Published

2019

5. Experimental Evolution of Escherichia coli K-12 at High pH and with RpoS Induction.

Author

Hamdallah, Issam, Torok, Nadia, Bischof, Katarina M., Majdalani, Nadim, Chadalavada, Sriya, Mdluli, Nonto, Creamer, Kaitlin E., Clark, Michelle, Holdener, Chase, Basting, Preston J., Gottesman, Susan, and Slonczewski, Joan L.

Subjects

*ESCHERICHIA coli, *GENETIC transcription, *BACTERIAL mutation, *HYDROGEN-ion concentration, *DNA-binding proteins, *GENETIC transcription regulation

Abstract

Experimental evolution of Escherichia coli K-12 W3110 by serial dilutions for 2,200 generations at high pH extended the range of sustained growth from pH 9.0 to pH 9.3. pH 9.3-adapted isolates showed mutations in DNA-binding regulators and envelope proteins. One population showed an IS1 knockout of phoB (encoding the positive regulator of the phosphate regulon). A phoB::kanR knockout increased growth at high pH. phoB mutants are known to increase production of fermentation acids, which could enhance fitness at high pH. Mutations in pcnB [poly(A) polymerase] also increased growth at high pH. Three out of four populations showed deletions of torI, an inhibitor of TorR, which activates expression of torCAD (trimethylamine N-oxide respiration) at high pH. All populations showed point mutations affecting the stationary-phase sigma factor RpoS, either in the coding gene or in genes for regulators of RpoS expression. RpoS is required for survival at extremely high pH. In our microplate assay, rpoS deletion slightly decreased growth at pH 9.1. RpoS protein accumulated faster at pH 9 than at pH 7. The RpoS accumulation at high pH required the presence of one or more antiadaptors that block degradation (IraM, IraD, and IraP). Other genes with mutations after high-pH evolution encode regulators, such as those encoded by yobG (mgrB) (PhoPQ regulator), rpoN (nitrogen starvation sigma factor), malI, and purR, as well as envelope proteins, such as those encoded by ompT and yahO. Overall, E. coli evolution at high pH selects for mutations in key transcriptional regulators, including phoB and the stationary-phase sigma factor RpoS. [ABSTRACT FROM AUTHOR]

Published

2018