Supreme activity of gramicidin S against resistant, persistent and biofilm cells of staphylococci and enterococci

Berditsch, Marina; Afonin, Sergii; Reuster, J.; Lux, Hannah; Schkolin, Kristina; Babii, Oleg; Radchenko, Dmytro S.; Abdullah, Issah; William, Nicola; Middel, Volker; Strähle, Uwe; Nelson, Andrew; Valkó, Klára; Ulrich, Anne S.

doi:10.1038/s41598-019-54212-z

Cited by 36 publications

(27 citation statements)

References 77 publications

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“…Pretreatment with sublethal concentations of antibiotics substantially increased the levels of persister cells (Johnson and Levin, 2013). Furthermore, in planktonic bacteria, exposure to subinhibitory concentrations of antibiotics induced switching to a biofilm lifestyle (Berditsch et al, 2019). SOS induction has also been shown to enhance the expression of fibronectin-binding protein (Bisognano et al, 2004) that facilitates attachment to host cells and biofilm formation (McCourt et al, 2014).…”

Section: Staphylococcus Aureusmentioning

confidence: 99%

The DNA Damage Inducible SOS Response Is a Key Player in the Generation of Bacterial Persister Cells and Population Wide Tolerance

2020

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Population-wide tolerance and persisters enable susceptible bacterial cells to endure hostile environments, including antimicrobial exposure. The SOS response can play a significant role in the generation of persister cells, population-wide tolerance, and shielding. The SOS pathway is an inducible DNA damage repair system that is also pivotal for bacterial adaptation, pathogenesis, and diversification. In addition to the two key SOS regulators, LexA and RecA, some other stressors and stress responses can control SOS factors. Bacteria are exposed to DNA-damaging agents and other environmental and intracellular factors, including cigarette smoke, that trigger the SOS response at a number of sites within the host. The Escherichia coli TisB/IstR module is as yet the only known SOS-regulated toxin-antitoxin module involved in persister formation. Nevertheless, the SOS response plays a key role in the formation of biofilms that are highly recalcitrant to antimicrobials and can be abundant in persisters. Furthermore, the dynamic biofilm environment generates DNA-damaging factors that trigger the SOS response within the biofilm, fueling bacterial adaptation and diversification. This review highlights the SOS response in relation to antimicrobial recalcitrance to antimicrobials in four clinically significant species, Escherichia coli, Pseudomonas aeruginosa, Staphylococcus aureus, and Mycobacterium tuberculosis.

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Section: Staphylococcus Aureusmentioning

confidence: 99%

The DNA Damage Inducible SOS Response Is a Key Player in the Generation of Bacterial Persister Cells and Population Wide Tolerance

2020

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“…Bacterial cells were then fixed with 2.5 % (w/v) glutaraldehyde at 4°C for 6 h. Before centrifugation at 8000 × g for 3 min, the cells were mixed by gently inverting the tube up and down for several minutes to prevent clumping of the cells. After three washes with PBS, the bacterial pellets were dehydrated for 15 min with a series of graded ethanol solutions (30,50,70,80, 90 and 100 %), the cells were mixed and centrifuged at 8000 × g for 3 min. Following dehydration, the dried bacterial cells were transferred to dry alcohol.…”

Section: Cp-mentioning

confidence: 99%

“…[10,21,28] The aforementioned GS, a well-known AMP obtained from bacteria, is active against a wide range of Gram-positive and Gram-negative bacteria, as well as viruses, fungi and tumors. [10,[29][30][31] Structurally, it is a cyclodecapeptide with the primary sequence cyclo-(VOL D FP) 2 (where O stands for ornithine), which adopts a rigid C 2 -symmetric β-hairpin structure (Figure 1, left panel). The global conformation is constrained by four intra-molecular H-bonds with four hydrophobic side-chains (Val and Leu) positioned on the opposite face from the two Orn cationic side chains, resulting in a strong amphiphilicity.…”

Section: Introductionmentioning

confidence: 99%

Gramicidin‐S‐Inspired Cyclopeptidomimetics as Potent Membrane‐Active Bactericidal Agents with Therapeutic Potential

Wen

Huang

et al. 2020

ChemMedChem

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Antimicrobial peptides (AMPs) are promising antibacterial agents often hindered by their undesired hemolytic activity. Inspired by gramicidin S (GS), a well‐known cyclodecapeptide, we synthesized a panel of antibacterial cyclopeptidomimetics using β,γ‐diamino acids (β,γ‐DiAAs). We observed that peptidomimetic CP‐2 displays a bactericidal activity similar to that of GS while possessing lower side‐effects. Moreover, extensive studies revealed that CP‐2 likely kills bacteria through membrane disruption. Altogether, CP‐2 is a promising membrane‐active antibiotic with therapeutic potential.

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“…Gramicidin S is a well-investigated cyclic decapeptide antibiotic with the sequence cyclo-(fPVOL)2. [22][23][24] Mono-modular GrsA (f) and tetramodular GrsB (PVOL) concatenate two molecules of pentapeptide fPVOL into gramicidin S. Here, in addition to the standard abbreviation of amino acids, letters in small case designate D-amino acids, "O" ornithine, and "O*" cyclized ornithine. Interruption of the gramicidin S assembly process leads to shunt products, for instance cyclo-(fP) 25 and fPVO* (Figure 1).…”

Section: Resultsmentioning

confidence: 99%

Engineering DNA templated nonribosomal peptide synthesis

Huang

Stephan

Kries

2020

Preprint

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Nanocontainers or macromolecular scaffolds for artificial biocatalytic cascades facilitate sequential enzyme reactions but diffusive escape of intermediates limits rate enhancement. Nonribosomal peptide synthetases (NRPS) naturally form gigantic assembly lines and prevent escape by covalently tethering intermediates. Here, we have built DNA-templated NRPS (DT-NRPS) by adding zinc finger tags to split NRPS modules. The zinc fingers direct the NRPS modules to 9-bp binding sites on a DNA strand, where they form a catalytically active enzyme cascade. DT-NRPS outperform previously reported DNA templated enzyme cascades in terms of DNA acceleration which demonstrates that covalent intermediate channeling is possible along the DNA template. Attachment of assembly line enzymes to a DNA scaffold is a promising catalytic strategy for the sequence-controlled biosynthesis of nonribosomal peptides and other polymers.

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Supreme activity of gramicidin S against resistant, persistent and biofilm cells of staphylococci and enterococci

Cited by 36 publications

References 77 publications

The DNA Damage Inducible SOS Response Is a Key Player in the Generation of Bacterial Persister Cells and Population Wide Tolerance

The DNA Damage Inducible SOS Response Is a Key Player in the Generation of Bacterial Persister Cells and Population Wide Tolerance

Gramicidin‐S‐Inspired Cyclopeptidomimetics as Potent Membrane‐Active Bactericidal Agents with Therapeutic Potential

Engineering DNA templated nonribosomal peptide synthesis

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