To Fold or Not to Fold: Diastereomeric Optimization of an α-Helical Antimicrobial Peptide

Personne, Hippolyte; Paschoud, Thierry; Fulgencio, Sofia; Baeriswyl, Stéphane; Köhler, Thilo; van Delden, Christian; Stocker, Achim; Javor, Sacha; Reymond, Jean-Louis

doi:10.1021/acs.jmedchem.3c00460

Cited by 9 publications

(10 citation statements)

References 81 publications

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“…Peptoid units can be introduced during standard Fmoc solid-phase peptide synthesis (Fmoc-SPPS) using the so-called submonomer strategy, which consists in bromoacetylation of the N -terminus of the growing chain followed by substitution of the bromide using an excess of a primary amine, here isobutylamine for a leucine peptoid unit ( N Leu) or tert -butyl (4-aminobutyl)carbamate for a lysine peptoid unit ( N Lys). We prepared the eleven selected peptide–peptoid hybrids together with undecapeptides ln65 and ln69 , as well as the PrAMP oncocin, to be used as positive controls, using high-temperature (60 °C) semiautomated Fmoc-SPPS on Rink amide resin in DMF with di-isopropyl carbodiimide (DIC) and OxymaPure as coupling reagents as described previously. , Addition of amino acids was repeated twice, while acylation with bromoacetic acid and displacement with the primary amine were performed only once. All products were obtained in pure form by acidic cleavage and deprotection followed by preparative reversed-phase HPLC (Scheme ).…”

Section: Resultsmentioning

confidence: 99%

Antimicrobial Peptide–Peptoid Hybrids with and without Membrane Disruption

Bonvin,

Personne,

Paschoud

et al. 2023

ACS Infect. Dis.

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Among synthetic analogues of antimicrobial peptides (AMPs) under investigation to address antimicrobial resistance, peptoids ( N -alkylated oligoglycines) have been reported to act both by membrane disruption and on intracellular targets. Here we gradually introduced peptoid units into the membrane-disruptive undecapeptide KKLLKLLKLLL to test a possible transition toward intracellular targeting. We found that selected hybrids containing up to five peptoid units retained the parent AMP’s α-helical folding, membrane disruption, and antimicrobial effects against Gram-negative bacteria including multidrug-resistant (MDR) strains of Pseudomonas aeruginosa and Klebsiella pneumoniae while showing reduced hemolysis and cell toxicities. Furthermore, some hybrids containing as few as three peptoid units as well as the full peptoid lost folding, membrane disruption, hemolysis, and cytotoxicity but displayed strong antibacterial activity under dilute medium conditions typical for proline-rich antimicrobial peptides (PrAMPs), pointing to intracellular targeting. These findings parallel previous reports that partially helical amphiphilic peptoids are privileged oligomers for antibiotic development.

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Section: Resultsmentioning

confidence: 99%

Antimicrobial Peptide–Peptoid Hybrids with and without Membrane Disruption

Bonvin,

Personne,

Paschoud

et al. 2023

ACS Infect. Dis.

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“…Remarkably, for those AMPs in both models 1 and 2, the impact of “helix breakers” on the structural and biological properties varies depending on each case. For example, stereorandomized derivative 23 of peptide 21 and its all‐D‐enantiomeric 22 ( both in model 1A and 2B) , the antibacterial activity was only slightly decreased whereas the minimum hemolysis concentration (MHC) was notably increased, thus indicating a significant improvement in selectivity [4a] . This interesting data suggested that many mutants among all the 1024 possible diastereometers that have better activity than both peptides 21 and 22 .…”

Section: The Influence Of Amphipathic Design To the Structure And Act...mentioning

confidence: 90%

“…This interesting data suggested that many mutants among all the 1024 possible diastereometers that have better activity than both peptides 21 and 22 . Then, a diastereomeric series of 21 was prepared to further examine the structure‐activity relationships [4a] . In terms of secondary structure, there are two directions observed.…”

Section: The Influence Of Amphipathic Design To the Structure And Act...mentioning

confidence: 99%

“…Additionally, diastereomeric optimization are demonstrated to improve the pharmacological properties of helical AMPs, including proteolytic resistance, antimicrobial potency and reduced toxicity [4a,b] . Nevertheless, a major drawback arises from the enormous number of possible mutant sequences.…”

Section: Amphipathic Design and Structural Modification Approachesmentioning

confidence: 99%

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The amphipathic design in helical antimicrobial peptides

Bui Thi Phuong,

Doan Ngan,

Le Huy

et al. 2024

ChemMedChem

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Amphipathicity is a critical characteristic of helical antimicrobial peptides (AMPs). The hydrophilic region, primarily composed of cationic residues, plays a pivotal role in the initial binding to negatively charged components on bacterial membranes through electrostatic interactions. Subsequently, the hydrophobic region interacts with hydrophobic components, inducing membrane perturbation, ultimately leading to cell death, or inhibiting intracellular function. Due to the extensive diversity of natural and synthetic AMPs with regard to the design of amphipathicity, it is complicated to study the structure‐activity relationships. Therefore, this work aims to categorize the common amphipathic design and investigate their impact on the biological properties of AMPs. Besides, the connection between current structural modification approaches and amphipathic styles was also discussed.

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“…In the context of developing computational tools for new modalities including beyond-Ro5 molecules [ 24 , 25 ], in our case for peptides with variable chain topology and stereochemistry [ 26 – 28 ], we have adapted molecular fingerprints based on atom-pairs [ 29 – 32 ] for large molecules such as peptides and proteins [ 33 – 35 ]. In particular, we combined atom-pair analysis and circular substructures as encoded by the Morgan fingerprint ECFP4 [ 36 , 37 ], with the principle of data compression using MinHashing [ 38 – 41 ], to design MAP4, a MinHashed Atom-Pair fingerprint.…”

Section: Introductionmentioning

confidence: 99%

One chiral fingerprint to find them all

Orsi,

Reymond

2024

J Cheminform

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Molecular fingerprints are indispensable tools in cheminformatics. However, stereochemistry is generally not considered, which is problematic for large molecules which are almost all chiral. Herein we report MAP4C, a chiral version of our previously reported fingerprint MAP4, which lists MinHashes computed from character strings containing the SMILES of all pairs of circular substructures up to a diameter of four bonds and the shortest topological distance between their central atoms. MAP4C includes the Cahn-Ingold-Prelog (CIP) annotation (R, S, r or s) whenever the chiral atom is the center of a circular substructure, a question mark for undefined stereocenters, and double bond cis–trans information if specified. MAP4C performs slightly better than the achiral MAP4, ECFP and AP fingerprints in non-stereoselective virtual screening benchmarks. Furthermore, MAP4C distinguishes between stereoisomers in chiral molecules from small molecule drugs to large natural products and peptides comprising thousands of diastereomers, with a degree of distinction smaller than between structural isomers and proportional to the number of chirality changes. Due to its excellent performance across diverse molecular classes and its ability to handle stereochemistry, MAP4C is recommended as a generally applicable chiral molecular fingerprint. Scientific contribution The ability of our chiral fingerprint MAP4C to handle stereoisomers from small molecules to large natural products and peptides is unprecedented and opens the way for cheminformatics to include stereochemistry as an important molecular parameter across all fields of molecular design. Graphical Abstract

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To Fold or Not to Fold: Diastereomeric Optimization of an α-Helical Antimicrobial Peptide

Cited by 9 publications

References 81 publications

Antimicrobial Peptide–Peptoid Hybrids with and without Membrane Disruption

Antimicrobial Peptide–Peptoid Hybrids with and without Membrane Disruption

The amphipathic design in helical antimicrobial peptides

One chiral fingerprint to find them all

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