Mode of Action of the Monobactam LYS228 and Mechanisms Decreasing
            <i>In Vitro</i>
            Susceptibility in Escherichia coli and Klebsiella pneumoniae

Dean, Charles R.; Barkan, David T.; Bermingham, Alun; Blais, Johanne; Casey, Fergal; Casarez, Anthony; Fuller, John; Jones, Adriana K.; Li, Cindy; López, Sara; Metzger, Louis E.; Mostafavi, Mina; Prathapam, Ramadevi; Rasper, Dita; Reck, Folkert; Ruzin, Alexey; Shaul, Jacob; Shen, Xiaoyu; Simmons, Robert L.; Skewes-Cox, Peter; Takeoka, Kenneth T.; Tamrakar, Pramila; Uehara, Tsuyoshi; Wei, Jun-Rong

doi:10.1128/aac.01200-18

Cited by 31 publications

(23 citation statements)

References 60 publications

(65 reference statements)

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“…The MIC of LYS228 increased to 8 and 32 g/ml for these mutants (NB29289-CDK0033 and CDK0034) (Table 1), and again LYS228 susceptibility was restored by the addition of avibactam (Table 1). It should be noted that no mpl mutations were isolated from several non-bla DHA-1 K. pneumoniae isolates during single-step selections described in an accompanying report (33), strengthening the association of mpl mutations with bla DHA-1 . Mpl is UDP-N-acetylmuramate:L-alanyl-␥-D-glutamyl-meso-diaminopimelate ligase, involved in peptidoglycan recycling (34,35), and its mutational loss may induce expression of bla DHA-1 via changes in peptidoglycan intermediates sensed by the plasmid-encoded AmpR regulator.…”

mentioning

confidence: 54%

Impact of Induciblebla_DHA-1on Susceptibility of Klebsiella pneumoniae Clinical Isolates to LYS228 and Identification of ChromosomalmplandampDMutations Mediating Upregulation of Plasmid-Bornebla_DHA-1Expression

Jones

Ranjitkar

López

et al. 2018

Antimicrob Agents Chemother

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Twenty-three () clinical isolates exhibited a range of susceptibilities to LYS228, with MICs of ≥8 μg/ml for 9 of these. Mutants with decreased susceptibility to LYS228 and upregulated expression of were selected from representative isolates. These had mutations in the chromosomal peptidoglycan recycling gene or Preexisting mutations were also found in some of the clinical isolates examined, and these had strongly upregulated expression of .

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confidence: 54%

Impact of Induciblebla_DHA-1on Susceptibility of Klebsiella pneumoniae Clinical Isolates to LYS228 and Identification of ChromosomalmplandampDMutations Mediating Upregulation of Plasmid-Bornebla_DHA-1Expression

Jones

Ranjitkar

López

et al. 2018

Antimicrob Agents Chemother

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“…To our knowledge these modifications are the only mutations contributing to β-lactams reported in natural E. coli isolates 19,25 . Nevertheless, the A413V mutation found in association with three types of insertions, has recently been selected during serial passages of E. coli in the presence of aztreonam and shown to lead to a four-fold decreased susceptibility to this antibiotic 38 . This result is in agreement with our prediction that this mutation might contribute to resistance to β-lactams of isolates carrying YRIK, YTIP or YRIP insertions as we have shown for the two SNPs associated with the YRIN duplication (Fig.…”

Section: Discussionmentioning

confidence: 99%

“…ftsI mutations were also found to be selected during in vitro evolution in the presence of ertapenem but not meropenem 43 . However, other β-lactams like aztreonam might also have contributed to the selection of these combinations of mutations 38 .…”

Section: Discussionmentioning

confidence: 99%

Stepwise evolution and convergent recombination underlie the global dissemination of carbapenemase-producingEscherichia coli

Patiño-Navarrete

Rosinski‐Chupin

Cabanel

et al. 2018

Preprint

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26Carbapenem-resistant Enterobacteriaceae are considered by WHO as "critical" priority 27 pathogens for which novel antibiotics are urgently needed. The dissemination of 28 carbapenemase-producing Escherichia coli (CP-Ec) in the community is a major public 29 health concern. However, the global molecular epidemiology of CP-Ec isolates, as well as 30 the genetic bases for the emergence and global dissemination of specific lineages, 31 remain largely unknown. Here, by combining a thorough genomic and evolutionary 32 analysis of Ec ST410 isolates with a broad analysis of 12,584 E. coli and Shigella 33 genomes, we showed that the fixation of carbapenemase genes depends largely on a 34 combination of mutations in ftsI encoding the penicillin binding protein 3 and in the 35 porin genes ompC and ompF. Mutated ftsI genes and a specific ompC allele inducing 36 reduced susceptibility to diverse β-lactams spread across the species by recombination. 37The selection of CP-Ec lineages able to disseminate is more complex than the mere 38 acquisition of carbapenemase genes. 39 40 41 Antibiotic resistance is one of the most urgent public health concerns. The 42 increasing rate in antimicrobial resistances worldwide suggests a bleak outlook in terms 43 of morbidity, mortality and economic loss 1 . Carbapenems are one of the last resort 44 antibiotics used to treat infections caused by multidrug-resistant (MDR) Gram-negative 45 bacteria 2 . Dissemination of carbapenem-resistant Enterobacteriaceae (CRE) threatens 46 the efficacy of current treatment options. Carbapenem-resistance may result from a 47 combination of mutations leading to reduced permeability (e.g. porin deficiency) and 48 overexpression of an extended-spectrum β-lactamase (ESBL) or a cephalosporinase that 49 show a weak activity against carbapenems 3 . However, the main resistance mechanism is 50 the acquisition of a carbapenemase gene 4 . The major carbapenemases encountered in 51Enterobacteriaceae belong to Ambler class A (KPC-type), class B (metallo-β-lactamases 52 IMP, VIM-and NDM-types) or class D (OXA-48-like enzymes) 5 . As these carbapenemases 53 are now frequently encountered in Escherichia coli, carbapenemase-producing E. coli 54 (CP-Ec) might follow the same expansion and dissemination in hospitals and the 55 community as the one observed for CTX-M-type ESBL-producing E. coli isolates 6,7 . A 56 scenario feared by public health authorities. This is especially worrisome as these 57 isolates are usually resistant to multiple antibiotics. 58The epidemiology of CP-Ec is complex with geographical diversity in terms of 59 carbapenemase genes and of dominant lineages 4 . Most studies performed at national or 60 hospital levels point to a broad diversity of isolates as defined by multilocus sequence 61 typing (MLST), with some isolates belonging to a few dominant sequence types (STs) 62 like ST38, clonal complex (CC) 10 (ST10, ST167, ST617), ST101, ST131 and ST410 that 63 express different carbapenemases 4,[8][9][10][11][12][13][14] . However, their prevalence vari...

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“…Additionally, it has been modified to resist hydrolysis by most serine β lactamases in Enterobacteriaceae 68 . Cross resistance exists with aztreonam when non β lactamase mechanisms are involved (for example, upregulated efflux and/or porin downregulation, or mutations in PBP3 and the envelope stress response system) 69 .…”

Section: New Stand-alone β-Lactam Antibioticsmentioning

confidence: 99%

Critical analysis of antibacterial agents in clinical development

Theuretzbacher¹,

et al. 2020

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| The antibacterial agents currently in clinical development are predominantly derivatives of well-established antibiotic classes and were selected to address the class-specific resistance mechanisms and determinants that were known at the time of their discovery. Many of these agents aim to target the antibiotic-resistant priority pathogens listed by the WHO, including Gram-negative bacteria in the critical priority category, such as carbapenem-resistant Acinetobacter, Pseudomonas and Enterobacterales. Although some current compounds in the pipeline have exhibited increased susceptibility rates in surveillance studies that depend on geography, pre-existing cross-resistance both within and across antibacterial classes limits the activity of many of the new agents against the most extensively drug-resistant (XDR) and pan-drug-resistant (PDR) Gram-negative pathogens. In particular, cross-resistance to unrelated classes may occur by co-selection of resistant strains, thus leading to the rapid emergence and subsequent spread of resistance. There is a continued need for innovation and new-class antibacterial agents in order to provide effective therapeutic options against infections specifically caused by XDR and PDR Gram-negative bacteria. ✉

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Mode of Action of the Monobactam LYS228 and Mechanisms Decreasing In Vitro Susceptibility in Escherichia coli and Klebsiella pneumoniae

Cited by 31 publications

References 60 publications

Impact of Induciblebla_DHA-1on Susceptibility of Klebsiella pneumoniae Clinical Isolates to LYS228 and Identification of ChromosomalmplandampDMutations Mediating Upregulation of Plasmid-Bornebla_DHA-1Expression

Impact of Induciblebla_DHA-1on Susceptibility of Klebsiella pneumoniae Clinical Isolates to LYS228 and Identification of ChromosomalmplandampDMutations Mediating Upregulation of Plasmid-Bornebla_DHA-1Expression

Stepwise evolution and convergent recombination underlie the global dissemination of carbapenemase-producingEscherichia coli

Critical analysis of antibacterial agents in clinical development

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Mode of Action of the Monobactam LYS228 and Mechanisms Decreasing In Vitro Susceptibility in Escherichia coli and Klebsiella pneumoniae

Cited by 31 publications

References 60 publications

Impact of InducibleblaDHA-1on Susceptibility of Klebsiella pneumoniae Clinical Isolates to LYS228 and Identification of ChromosomalmplandampDMutations Mediating Upregulation of Plasmid-BorneblaDHA-1Expression

Impact of InducibleblaDHA-1on Susceptibility of Klebsiella pneumoniae Clinical Isolates to LYS228 and Identification of ChromosomalmplandampDMutations Mediating Upregulation of Plasmid-BorneblaDHA-1Expression

Stepwise evolution and convergent recombination underlie the global dissemination of carbapenemase-producingEscherichia coli

Critical analysis of antibacterial agents in clinical development

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Product

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Impact of Induciblebla_DHA-1on Susceptibility of Klebsiella pneumoniae Clinical Isolates to LYS228 and Identification of ChromosomalmplandampDMutations Mediating Upregulation of Plasmid-Bornebla_DHA-1Expression

Impact of Induciblebla_DHA-1on Susceptibility of Klebsiella pneumoniae Clinical Isolates to LYS228 and Identification of ChromosomalmplandampDMutations Mediating Upregulation of Plasmid-Bornebla_DHA-1Expression