Porin Loss Impacts the Host Inflammatory Response to Outer Membrane Vesicles of Klebsiella pneumoniae

Turner, Kelli L.; Cahill, Bethaney K.; Dilello, Sarah K.; Gutel, Dedra; Brunson, Debra N; Albertí, Sebastián; Ellis, Terri N.

doi:10.1128/aac.01627-15

Cited by 28 publications

(16 citation statements)

References 60 publications

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“…The β-lactam antibiotic must pass through the traverse porin channel in the outer membrane to access the PBP of the inner plasma membrane. However, proteins produced by mutations in porin-encoding genes or porin loss show lower permeability to β-lactam antibiotics 42 , 43 . Efflux pumps can export a wide range of substrates from the periplasm to the surrounding environment 44 , thus overproduction of efflux pump can augment the resistance of β-lactam antibiotics 45 .…”

Section: Discussionmentioning

confidence: 99%

Outer membrane vesicles from β-lactam-resistant Escherichia coli enable the survival of β-lactam-susceptible E. coli in the presence of β-lactam antibiotics

Kim

Park

et al. 2018

Sci Rep

116

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Outer membrane vesicles (OMVs) containing various bacterial compounds are released from mainly gram-negative bacteria. Secreted OMVs play important roles in the ability of a bacterium to defend itself, and thus contribute to the survival of bacteria in a community. In this study, we collected OMVs from β-lactam antibiotic-resistant Escherichia coli established by conjugation assay and the parental β-lactam antibiotic-susceptible strain, and performed comparative proteomic analysis to examine whether these OMVs carried β-lactam-resistant compounds. We also investigated whether both types of OMVs could protect susceptible cells from β-lactam-induced death and/or directly degrade β-lactam antibiotics. Several proteins that can be involved in degrading β-lactam antibiotics were more abundant in OMVs from β-lactam-resistant E. coli, and thus OMVs from β-lactam resistant E. coli could directly and dose-dependently degrade β-lactam antibiotics and fully rescue β-lactam-susceptible E. coli and other bacterial species from β-lactam antibiotic-induced growth inhibition. Taken together, present study demonstrate that OMVs from β-lactam-resistant E. coli play important roles in survival of antibiotic susceptible bacteria against β-lactam antibiotics. This finding may pave the way for new efforts to combat the current global spread of antibiotic resistances, which is considered to be a significant public health threat.

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Section: Discussionmentioning

confidence: 99%

Outer membrane vesicles from β-lactam-resistant Escherichia coli enable the survival of β-lactam-susceptible E. coli in the presence of β-lactam antibiotics

Kim

Park

et al. 2018

Sci Rep

116

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“…In our study, ESBL-producing isolates and AmpC enzyme-producing isolates exhibited different resistance patterns with higher resistance rate to ceftriaxone and cefepime vs. higher resistance rates to ceftazidime and cefoxitin, respectively ( Table 2). Regardless of whether the isolate was ESBL-or non-ESBL-producing, the carbapenem-resistant isolates carried bla DHA-1 and an insertion in both ompK35 and ompK36 genes, exhibiting the highest MIC to carbapenems ( and a significant decrease in proinflammatory cytokine levels [45]. Further, the loss of OmpK35 is associated with resistance to lipophilic (benzylpenicillin) and large (cefepime) compounds [46].…”

Section: Discussionmentioning

confidence: 98%

Insertion Sequence-Dependent <i>OmpK</i>36 Mutation Associated Ertapenem Resistance in Clinical <i>Klebsiella pneumoniae</i>

Lee¹,

Huang²,

Hsiao³

et al. 2018

AiM

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Extended-spectrum β-lactamases (ESBLs) and/or AmpC enzymes combined with deficiency of porins OmpK35 and OmpK36 are important for the development of carbapenem-resistant Klebsiella pneumoniae. We characterized the clinical K. pneumoniae human isolates and investigated the effect of meropenem induction on the ompK35 and ompK36 mutation to develop carbapenem resistance from six carbapenem-susceptible ESBL-producing K. pneumoniae strains. 163 clinical K. pneumoniae isolates were grouped mostly into the ESBL + AmpC (44.2%) and ESBL (42.9%) phenotypes. The resistance rate differed between cephalosporins (52.1% for cefepime -97.5% for cefotaxime) and carbapenems (16% for meropenem -28.2% for imipenem) (P < 0.001). The ESBL group showed the lowest resistance to cefoxitin and cefepime and all carbapenems, whereas the AmpC group exhibited the lowest resistance to cefepime and the highest resistance to all carbapenems. PCR amplification identified bla TEM , bla SHV , bla CTX-M-3-like , and bla CTX-M-14-like of AmpA β-lactamase genes and bla DHA and bla CMY of AmpC β-lactamase genes. Compared to all 163 clinical isolates, the 56 carbapenem-resistant isolates carried less frequently of bla TEM , bla CTXM-14-like , and bla CTXM-3-like and more frequently of bla DHA-1 and bla C-MY-2 . The carbapenem-resistant isolates differed in prevalence against imipenem, ertapenem, and meropenem and lacked OmpK35 more frequently than OmpK36, but abnormal PCR amplicons were detected fewer in the Omp K35-deficient group than in the OmpK36-deficient group (32.5% vs. 68.4%,

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“…In K. pneumoniae , loss of porins OmpK 35 and OmpK 36, homologs of OmpC and OmpF, respectively, showed different protein composition of outer membrane vesicles. These vesicles were found to induce secretion of extremely low levels of proinflammatory cytokine 50 . Indeed, low cytokine secretion may be an evasion mechanism for bacteria to escape from the host immune response.…”

Section: Discussionmentioning

confidence: 99%

Fine-tuning carbapenem resistance by reducing porin permeability of bacteria activated in the selection process of conjugation

Kong

Pan

et al. 2018

Sci Rep

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Antibiotic resistance is an emerging public health issue. Plasmids are one of the popular carriers to disseminate resistance genes among pathogens. However, the response of plasmid-carrying bacteria to antibiotic treatment and how these bacteria evolve to increase their resistance remain elusive. In this study, we conjugated plasmid pNDM-HK to E. coli J53 recipient cells and selected survivors using different concentrations of the broad spectrum antibiotic meropenem. After selection, transconjugants conferred varying minimum inhibitory concentrations with respect to carbapenems. We sequenced and compared the transcriptomes of transconjugants that exhibited distinct carbapenem susceptibilities, and found that the loss of outer membrane proteins led to antibiotic resistance. Moreover, we identified a novel mutation, G63S, in transcription factor OmpR which moderates the expression of outer membrane proteins. The loss of porins was due to incapability of phosphorylation, which is essential for porin transcription and carbapenem resistance. We also characterized other genes that are regulated by ompR in this mutant, which contributed to bacterial antibiotic resistance. Overall, our studies suggest antibiotic pressure after conjugation might be an alternative pathway to promote antimicrobial resistance.

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Porin Loss Impacts the Host Inflammatory Response to Outer Membrane Vesicles of Klebsiella pneumoniae

Cited by 28 publications

References 60 publications

Outer membrane vesicles from β-lactam-resistant Escherichia coli enable the survival of β-lactam-susceptible E. coli in the presence of β-lactam antibiotics

Outer membrane vesicles from β-lactam-resistant Escherichia coli enable the survival of β-lactam-susceptible E. coli in the presence of β-lactam antibiotics

Insertion Sequence-Dependent <i>OmpK</i>36 Mutation Associated Ertapenem Resistance in Clinical <i>Klebsiella pneumoniae</i>

Fine-tuning carbapenem resistance by reducing porin permeability of bacteria activated in the selection process of conjugation

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Porin Loss Impacts the Host Inflammatory Response to Outer Membrane Vesicles of Klebsiella pneumoniae

Cited by 28 publications

References 60 publications

Outer membrane vesicles from β-lactam-resistant Escherichia coli enable the survival of β-lactam-susceptible E. coli in the presence of β-lactam antibiotics

Outer membrane vesicles from β-lactam-resistant Escherichia coli enable the survival of β-lactam-susceptible E. coli in the presence of β-lactam antibiotics

Insertion Sequence-Dependent &lt;i&gt;OmpK&lt;/i&gt;36 Mutation Associated Ertapenem Resistance in Clinical &lt;i&gt;Klebsiella pneumoniae&lt;/i&gt;

Fine-tuning carbapenem resistance by reducing porin permeability of bacteria activated in the selection process of conjugation

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Insertion Sequence-Dependent <i>OmpK</i>36 Mutation Associated Ertapenem Resistance in Clinical <i>Klebsiella pneumoniae</i>