The Lipopeptide Antibiotic Friulimicin B Inhibits Cell Wall Biosynthesis through Complex Formation with Bactoprenol Phosphate

Schneider, Tanja; Gries, Klara; Josten, Michaele; Wiedemann, Imke; Pelzer, Stefan; Labischinski, Harald; Sahl, Hans Georg

doi:10.1128/aac.01040-08

Cited by 149 publications

(152 citation statements)

References 44 publications

(43 reference statements)

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“…The members of this group also share one action mechanism, which consists of binding and sequestering undecaprenol phosphate, a bacterial membrane constituent that is an essential carrier coenzyme in the assembly and membrane translocation of peptidoglycan precursors. This was shown first for amphomycin 28,29 and more recently for friulimycin 30 and laspartomycin. 31 Structural homology is greater within each group, yet it is also considerable between them (cf.…”

Section: Relationship To Other Calcium-dependent Lipopeptide Antibioticsmentioning

confidence: 81%

The action mechanism of daptomycin

Taylor

Palmer

2016

Bioorganic & Medicinal Chemistry

204

161

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Daptomycin is a lipopeptide antibiotic produced by the soil bacterium Streptomyces roseosporus that is clinically used to treat severe infections with Grampositive bacteria. In this review, we discuss the mode of action of this important antibiotic. Although daptomycin is structurally related to amphomycin and similar lipopeptides that inhibit peptidoglycan biosynthesis, experimental studies have not produced clear evidence that daptomycin shares their action mechanism. Instead, the best characterized effect of daptomycin is the permeabilization and depolarization of the bacterial cell membrane. This activity, which can account for daptomycin's bactericidal effect, correlates with the level of phosphatidylglycerol (PG) in the membrane. Accordingly, reduced synthesis of PG or its increased conversion to lysyl-PG promotes bacterial resistance to daptomycin. While other resistance mechanisms suggest that daptomycin may indeed directly interfere with cell wall synthesis or cell division, such effects still await direct experimental confirmation. Daptomycin's complex structure and biosynthesis have hampered the analysis of its structure activity relationships. Novel methods of total synthesis, including a recent one that is carried out entirely on a solid phase, will enable a more thorough and systematic exploration of the sequence space.

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Section: Relationship To Other Calcium-dependent Lipopeptide Antibioticsmentioning

confidence: 81%

The action mechanism of daptomycin

Taylor

Palmer

2016

Bioorganic & Medicinal Chemistry

204

161

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“…At present, daptomycin is the only clinically used CDA, and its mode of action is the topic of ongoing investigation 6, 7, 8, 9. By comparison, the structurally similar CDAs laspartomycin C, friulimycin B, tsushimycin, and amphomycin have more clearly understood antibacterial mechanisms 10, 11, 12, 13, 14. It was recently reported that laspartomycin C forms a high‐affinity complex ( K d =7.3±3.8 n m ) with the bacterial cell wall precursor undecaprenyl phosphate (C 55 ‐P) and in doing so inhibits peptidoglycan biosynthesis, ultimately leading to cell death 14.…”

mentioning

confidence: 99%

A High‐Resolution Crystal Structure that Reveals Molecular Details of Target Recognition by the Calcium‐Dependent Lipopeptide Antibiotic Laspartomycin C

et al. 2017

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The calcium‐dependent antibiotics (CDAs) are an important emerging class of antibiotics. The crystal structure of the CDA laspartomycin C in complex with calcium and the ligand geranyl‐phosphate at a resolution of 1.28 Å is reported. This is the first crystal structure of a CDA bound to its bacterial target. The structure is also the first to be reported for an antibiotic that binds the essential bacterial phospholipid undecaprenyl phosphate (C55‐P). These structural insights are of great value in the design of antibiotics capable of exploiting this unique bacterial target.

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“…19 The scenario is even more disappointing for compounds targeting Gram-negative pathogens, in which old drugs have been revamped for new uses, and none of them has reached phase III yet (Table 1). Ceftazidime is a marketed cephalosporin being developed in combination with NXL104, a representative of a new class of b-lactamase inhibitors, 20 which renders cephalosporin effective against most b-lactamase-producing enterobacteria.…”

mentioning

confidence: 99%

Antibiotic discovery in the twenty-first century: current trends and future perspectives

Donadio¹,

Maffioli²,

Monciardini³

et al. 2010

J Antibiot

214

122

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New antibiotics are necessary to treat microbial pathogens that are becoming increasingly resistant to available treatment. Despite the medical need, the number of newly approved drugs continues to decline. We offer an overview of the pipeline for new antibiotics at different stages, from compounds in clinical development to newly discovered chemical classes. Consistent with historical data, the majority of antibiotics under clinical development are natural products or derivatives thereof. However, many of them also represent improved variants of marketed compounds, with the consequent risk of being only partially effective against the prevailing resistance mechanisms. In the discovery arena, instead, compounds with promising activities have been obtained from microbial sources and from chemical modification of antibiotic classes other than those in clinical use. Furthermore, new natural product scaffolds have also been discovered by ingenious screening programs. After providing selected examples, we offer our view on the future of antibiotic discovery.

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The Lipopeptide Antibiotic Friulimicin B Inhibits Cell Wall Biosynthesis through Complex Formation with Bactoprenol Phosphate

Cited by 149 publications

References 44 publications

The action mechanism of daptomycin

The action mechanism of daptomycin

A High‐Resolution Crystal Structure that Reveals Molecular Details of Target Recognition by the Calcium‐Dependent Lipopeptide Antibiotic Laspartomycin C

Antibiotic discovery in the twenty-first century: current trends and future perspectives

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