Overcoming antibiotic resistance in Pseudomonas aeruginosa biofilms using glycopeptide dendrimers

Michaud, Gaëlle; Visini, Ricardo; Bergmann, Myriam; Salerno, Gianluca; Bosco, Rosa; Gillon, Émilie; Richichi, Barbara; Nativi, Cristina; Imberty, Anne; Stocker, Achim; Darbre, Tamis; Reymond, Jean‐Louis

doi:10.1039/c5sc03635f

Cited by 99 publications

(115 citation statements)

References 59 publications

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“…Others have also developed very potent LecA inhibitors through structural modifications and refinements, such as Reymond et al. (glycopeptide dendrimer, 2.5 n m , isothermal titration calorimetry (ITC)), Pieters et al. (rigid dimer, 28 n m , ITC), Imberty, Römer, Winssinger et al.…”

Section: Resultsmentioning

confidence: 99%

“…The activitieso fo ur glycoconjugates are comparable to the glycodendrimers reported by Roy et al (230 nm,S PR). [21] Others have also developed very potent LecA inhibitors through structural modifications andr efinements, such as Reymond et al (glycopeptide dendrimer,2 .5 nm,i sothermal titration calorimetry (ITC)), [22] Pieterse tal. (rigid dimer,2 8nm,I TC), [34] Imberty, Rçmer,W inssinger et al (glycopeptide dimer,8 2nm,I TC), [38]…”

Section: Resultsmentioning

confidence: 99%

“…[16] Another approach to enhancei nhibitor interaction to LecA is through multivalent binding. Because LecA is at etrameric lectin andt he two closest binding sites are separated by about 26 , [17] various artificial scaffolds including dendrimers, [11,[18][19][20][21][22][23][24] clusters, [12][13][14][25][26][27][28][29][30][31][32] and linear rigid spacers [33][34][35][36] have been exploited to present galactoside ligands to theb inding sites to enhancei nhibition activity. [37] In other cases, the artificial scaffoldsa re furtherf unctionalized to generate extra interactions with LecA for stronger binding.…”

Section: Introductionmentioning

confidence: 99%

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Development of Pseudomonas aeruginosa Lectin LecA Inhibitor by using Bivalent Galactosides Supported on Polyproline Peptide Scaffolds

Huang

Lin

Lai

et al. 2018

Chemistry An Asian Journal

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LecA is a galactose-binding tetrameric lectin from Pseudomonas aeruginosa involved in infection and biofilm formation. The emergent antibiotic resistance of P. aeruginosa has made LecA a promising pharmaceutical target to treat such infections. To develop LecA inhibitors, we exploit the unique helical structure of polyproline peptides to create a scaffold that controls the galactoside positions to fit their binding sites on LecA. With a modular scaffold design, both the galactoside ligands and the inter-ligand distance can be altered conveniently. We prepared scaffolds with spacings of 9, 18, 27, and 36 Å for ligand conjugation and found that glycopeptides with galactosides ligands three helical turns (27 Å) apart best fit LecA. In addition, we tested different galactose derivatives on the selected scaffold (27 Å) to improve the binding avidity to LecA. The results validate a new multivalent scaffold design and provide useful information for LecA inhibitor development.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Development of Pseudomonas aeruginosa Lectin LecA Inhibitor by using Bivalent Galactosides Supported on Polyproline Peptide Scaffolds

Huang

Lin

Lai

et al. 2018

Chemistry An Asian Journal

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“…In the course of investigating peptide dendrimers as enzyme models and for nucleic acids and drug delivery, [14 -18] we discovered compounds acting on bacteria, either in the form of glycopeptide dendrimers targeting lectins and capable of inhibiting biofilms, [19][20][21] or as polycationic dendrimers exerting membrane perturbation effects. We identified our first membrane disrupting antimicrobial peptide dendrimer (AMPD) by screening a combinatorial library using an off-bead Bacillus subtilis growth inhibition assay, [22 -24] which pointed to dendrimer bH1, a third generation (G3) dendrimer containing single hydrophobic residues in its branches and eight positive charges at the N-termini ( Figure 1, Table 1).…”

Section: Introductionmentioning

confidence: 99%

Antimicrobial Peptide Dendrimer Chimera

Siriwardena

Lüscher

Köhler

et al. 2019

Helvetica Chimica Acta

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We recently reported the discovery of antimicrobial peptide dendrimers (AMPDs) acting by a membrane‐disruptive mechanism against multidrug resistant pathogenic bacteria. Here, we combined amino acid sequence elements from different AMPDs with different activity profiles to form AMPD chimeras. By joining the outer branches of TNS18, an AMPD active against Pseudomonas aeruginosa, Acinetobacter baumannii and methicillin resistant Staphylococcus aureus, with the core of T7, another AMPD active against P. aeruginosa, A. baumannii and Klebsiella pneumoniae, we obtained AMPD chimera DC5 displaying all previously observed activities while retaining a similar mechanism of action. These experiments show that chimera design represents a useful strategy to improve the properties of AMPDs.

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“…[7] Thus,t he inhibition of these lectins provides ap romising way to dismantle the bacterium from the protective biofilm environment and restore immune defense and activity of antibiotics. [8] Current approaches to inhibit both lectins range from small molecules to multivalent structures and are summarized in recent reviews. [9] We focus on the development of small molecules and recently published various potent glycomimetic inhibitors for the high affinity lectin LecB as inhibitors of P. aeruginosa adhesion.…”

mentioning

confidence: 99%

Covalent Lectin Inhibition and Application in Bacterial Biofilm Imaging

et al. 2017

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Biofilm formation by pathogenic bacteria is a hallmark of chronic infections. In many cases, lectins play key roles in establishing biofilms. The pathogen Pseudomonas aeruginosa often exhibiting various drug resistances employs its lectins LecA and LecB as virulence factors and biofilm building blocks. Therefore, inhibition of the function of these proteins is thought to have potential in developing “pathoblockers” preventing biofilm formation and virulence. A covalent lectin inhibitor specific to a carbohydrate binding site is described for the first time. Its application in the LecA‐specific in vitro imaging of biofilms formed by P. aeruginosa is also reported.

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Overcoming antibiotic resistance in Pseudomonas aeruginosa biofilms using glycopeptide dendrimers

Abstract: Glycopeptide dendrimers targeting P. aeruginosa lectins yielded to crystallography and acted in synergy with tobramycin for biofilm inhibition and dispersal.

Cited by 99 publications

References 59 publications

Development of Pseudomonas aeruginosa Lectin LecA Inhibitor by using Bivalent Galactosides Supported on Polyproline Peptide Scaffolds

Development of Pseudomonas aeruginosa Lectin LecA Inhibitor by using Bivalent Galactosides Supported on Polyproline Peptide Scaffolds

Antimicrobial Peptide Dendrimer Chimera

Covalent Lectin Inhibition and Application in Bacterial Biofilm Imaging

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