Application of Virtual Screening to the Identification of New LpxC Inhibitor Chemotypes, Oxazolidinone and Isoxazoline

Lee, Patrick S.; Lapointe, Guillaume; Madera, Ann Marie; Simmons, Robert L.; Xu, Wei; Yifru, Aregahegn; Tjandra, Meiliana; Karur, Subramanian; Rico, Alice; Thompson, Katherine; Bojkovic, Jade; Xie, Lili; Uehara, Kyoko; Liu, Amy; Shu, Wei; Bellamacina, Cornelia; McKenney, David; Morris, Laura; Tonn, George; Osborne, Colin; Benton, Bret M.; McDowell, Laura; Fu, Jiping; Sweeney, Zachary K.

doi:10.1021/acs.jmedchem.8b01287

Cited by 21 publications

(26 citation statements)

References 32 publications

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“…1), and since then many others have been reported (7,18,19). Recent examples from our group include compound 1 (9) and compound 2 (oxazolidinone 13f), compound 3 (isoxazoline 25d), and compound 4 (isoxazoline 25e) described previously (12) (Fig. 1) that have potent in vitro activity against P. aeruginosa.…”

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confidence: 78%

“…Along with being a key factor in establishing the permeability barrier of the OM, LPS is also essential for growth and virulence in many Gram-negative pathogens such as Escherichia coli, Klebsiella pneumoniae, and Pseudomonas aeruginosa. Targets in the lipid A biosynthetic pathway, in particular LpxC (7)(8)(9)(10)(11)(12), or in the machinery that transports LPS and assembles it in the OM (13) have been the focus of intense drug discovery efforts. Early efforts to identify LpxC inhibitors yielded compounds that had activity against E. coli but not P. aeruginosa (14), raising the possibility that these inhibitors did not accumulate sufficiently in P. aeruginosa (as is often the case) or that LpxC was not essential in this pathogen.…”

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confidence: 99%

“…We also noted that in vitro passaging of cells in the presence of CHIR-090 can lead to cumulative and substantial reductions in susceptibility. Here, we used single-step mutant selections and passaging approaches, along with targeted and genome sequencing, to examine the role of efflux and nonefflux mechanisms in mediating decreased susceptibility to CHIR-090 and the more recently described LpxC inhibitors compound 1 (9), compound 2 (oxazolidinone 13f), compound 3 (isoxazoline 25d), and compound 4 (isoxazoline 25e) (12) (Fig. 1) that have potent in vitro activity against P. aeruginosa.…”

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confidence: 99%

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Mutations Reducing In Vitro Susceptibility to Novel LpxC Inhibitors in Pseudomonas aeruginosa and Interplay of Efflux and Nonefflux Mechanisms

Jones

Caughlan

Woods

et al. 2019

Antimicrob Agents Chemother

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Upregulated expression of efflux pumps, lpxC target mutations, LpxC protein overexpression, and mutations in fabG were previously shown to mediate single-step resistance to the LpxC inhibitor CHIR-090 in P. aeruginosa. Single-step selection experiments using three recently described LpxC inhibitors (compounds 2, 3, and 4) and mutant characterization showed that these mechanisms affect susceptibility to additional novel LpxC inhibitors. Serial passaging of P. aeruginosa wild-type and efflux pump-defective strains using the LpxC inhibitor CHIR-090 or compound 1 generated substantial shifts in susceptibility and underscored the interplay of efflux and nonefflux mechanisms. Whole-genome sequencing of CHIR-090 passage mutants identified efflux pump overexpression, fabG mutations, and novel mutations in fabF1 and in PA4465 as determinants of reduced susceptibility. Two new lpxC mutations, encoding A214V and G208S, that reduce susceptibility to certain LpxC inhibitors were identified in these studies, and we show that these and other target mutations differentially affect different LpxC inhibitor scaffolds. Lastly, the combination of target alteration (LpxCA214V) and upregulated expression of LpxC was shown to be tolerated in P. aeruginosa and could mediate significant decreases in susceptibility.

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confidence: 78%

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confidence: 99%

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Mutations Reducing In Vitro Susceptibility to Novel LpxC Inhibitors in Pseudomonas aeruginosa and Interplay of Efflux and Nonefflux Mechanisms

Jones

Caughlan

Woods

et al. 2019

Antimicrob Agents Chemother

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“…Since the discovery of L-161240 as the first LpxC inhibitor in the 1990s 11 , many LpxC inhibitors have been reported as antibacterial agents [6][7][8] . Most LpxC inhibitors share common structural features that mimic the natural Zn 2þ -binding substrate: (1) a hydroxamate head group, (2) a central linker, and (3) a lipophilic tail 12 . Among the well-characterised compounds, threonyl-hydroxamate derivatives, such as CHIR-12 and LPC-009, are representative LpxC inhibitors [13][14][15] .…”

Section: Introductionmentioning

confidence: 99%

Synthesis, antibacterial and anticancer activity, and docking study of aminoguanidines containing an alkynyl moiety

Deng

Song

2019

Journal of Enzyme Inhibition and Medicinal Chemistry

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Two series of aminoguanidines containing an alkynyl moiety were designed, synthesised, and screened for antibacterial and anticancer activities. Generally, the series 3a-3j with a 1,2-diphenylethyne exhibited better antibacterial activity than the other series (6a-6k) holding 1,4-diphenylbuta-1,3-diyne moiety antibacterial activity. Most compounds in series 3a-3j showed potent growth inhibition against the tested bacterial strains, with minimum inhibitory concentration (MIC) values in the range 0.25-8 mg/mL. Compound 3g demonstrated rapid and persistent bactericidal activity at 2 Â MIC. The resistance study revealed that resistance of the tested bacteria towards 3g is not easily developed. Molecular docking studies revealed that compounds 3g and 6e bind strongly to the LpxC and FabH enzymes. Moreover, excellent activity of selected compounds against the growth of cancer cell lines A549 and SGC7901 was also observed, with IC 50 values in the range 0.30-4.57 mg/mL. These findings indicate that compounds containing the aminoguanidine moiety are promising candidates for the development of new antibacterial and anticancer agents.

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“…17 Since lipid A is essential for growth and structural integrity of most Gram-negative bacteria, small molecule inhibitors of lipid A biosynthesis prevent growth or restore the activity of antibiotics with intracellular targets that could not otherwise be reached. 14–15, 18 Furthermore, inhibition of lipid A biosynthesis can reduce the levels of endotoxin that are released during antibiotic treatment. 19 Therefore, lipid A biosynthesis has been viewed as a promising target for the discovery of new antibacterials.…”

Section: Introductionmentioning

confidence: 99%

Two distinct mechanisms of small molecule inhibition of LpxA acyltransferase essential for lipopolysaccharide biosynthesis

Han¹,

Ma²,

Balibar³

et al. 2019

Preprint

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Application of Virtual Screening to the Identification of New LpxC Inhibitor Chemotypes, Oxazolidinone and Isoxazoline

Cited by 21 publications

References 32 publications

Mutations Reducing In Vitro Susceptibility to Novel LpxC Inhibitors in Pseudomonas aeruginosa and Interplay of Efflux and Nonefflux Mechanisms

Mutations Reducing In Vitro Susceptibility to Novel LpxC Inhibitors in Pseudomonas aeruginosa and Interplay of Efflux and Nonefflux Mechanisms

Synthesis, antibacterial and anticancer activity, and docking study of aminoguanidines containing an alkynyl moiety

Two distinct mechanisms of small molecule inhibition of LpxA acyltransferase essential for lipopolysaccharide biosynthesis

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