An amphipathic cyclic tetrapeptide scaffold containing halogenated β<sup>2,2</sup>‐amino acids with activity against multiresistant bacteria

Paulsen, Marianne Hagensen; Karlsen, Eskil André; Ausbacher, Dominik; Anderssen, Trude; Bayer, Annette; Ochtrop, Philipp; Hedberg, Christian; Haug, Tor; Sollid, Johanna U. Ericson; Strøm, Morten B.

doi:10.1002/psc.3117

Cited by 9 publications

(8 citation statements)

References 25 publications

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“…A recent study has described the incorporation of two halogenated α,α-disubstituted β 2,2 -amino acid residues [ 218 ] into an amphipathic cyclic tetrapeptide [ 219 ] ( Figure 8 ) with general sequence c(Lys-β2,2-Xaa-Lys), where Xaa = Lys, Gly, Ala, or Phe. Antimicrobial activity was in the low μg/mL concentration range against multi-resistant Gram-(+) and Gram-(-) strains, with little toxicity against human red blood cells, in particular for the halogenated analogues c(Lys-β 2,2 (4-CF 3 )-Phe-Lys) and c(Lys-β 2,2 (3,5-di-CF 3 )-Gly-Lys).…”

Section: Halogenated Ampsmentioning

confidence: 99%

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Natural and Synthetic Halogenated Amino Acids—Structural and Bioactive Features in Antimicrobial Peptides and Peptidomimetics

Mardirossian

Rubini

Adamo³

et al. 2021

Molecules

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The 3D structure and surface characteristics of proteins and peptides are crucial for interactions with receptors or ligands and can be modified to some extent to modulate their biological roles and pharmacological activities. The introduction of halogen atoms on the side-chains of amino acids is a powerful tool for effecting this type of tuning, influencing both the physico-chemical and structural properties of the modified polypeptides, helping to first dissect and then rationally modify features that affect their mode of action. This review provides examples of the influence of different types of halogenation in amino acids that replace native residues in proteins and peptides. Examples of synthetic strategies for obtaining halogenated amino acids are also provided, focusing on some representative compounds and their biological effects. The role of halogenation in native and designed antimicrobial peptides (AMPs) and their mimetics is then discussed. These are in the spotlight for the development of new antimicrobial drugs to counter the rise of antibiotic-resistant pathogens. AMPs represent an interesting model to study the role that natural halogenation has on their mode of action and also to understand how artificially halogenated residues can be used to rationally modify and optimize AMPs for pharmaceutical purposes.

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Section: Halogenated Ampsmentioning

confidence: 99%

“… In this figure, a hierarchical approach from peptide to peptidomimetic is resumed. ( A ) From SMAMPs [ 219 ]: a peptide scaffold was used to investigate the effect of halogenation and hydrophobicity. ( B ) Summary of SAR for peptidomimetics [ 220 ].…”

Section: Figures Schemes and Tablesmentioning

confidence: 99%

Natural and Synthetic Halogenated Amino Acids—Structural and Bioactive Features in Antimicrobial Peptides and Peptidomimetics

Mardirossian

Rubini

Adamo³

et al. 2021

Molecules

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“…So far, fluorination has received the most interest, though the studies tackling the link between fluorination and antimicrobial activity have led to somewhat inconclusive results. For example, introduction of hexafluoroleucine into magainin and buforin conferred enhanced antimicrobial activity and retained low hemolytic properties, while the presence of fluorine atoms and trifluoromethyl groups improved the potency of short cationic peptides 15 – 17 . By contrast, incorporation of hexafluoroleucine into protegrin analogs led to decreased potency, while lipopeptides with fluorinated tails demonstrated moderate antibacterial activity combined with pronounced hemolytic properties 18 , 19 .…”

Section: Introductionmentioning

confidence: 99%

Halogenation as a tool to tune antimicrobial activity of peptoids

Molchanova

Nielsen

Sørensen

et al. 2020

Sci Rep

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Antimicrobial peptides have attracted considerable interest as potential new class of antibiotics against multi-drug resistant bacteria. However, their therapeutic potential is limited, in part due to susceptibility towards enzymatic degradation and low bioavailability. Peptoids (oligomers of N-substituted glycines) demonstrate proteolytic stability and better bioavailability than corresponding peptides while in many cases retaining antibacterial activity. In this study, we synthesized a library of 36 peptoids containing fluorine, chlorine, bromine and iodine atoms, which vary by length and level of halogen substitution in position 4 of the phenyl rings. As we observed a clear correlation between halogenation of an inactive model peptoid and its increased antimicrobial activity, we designed chlorinated and brominated analogues of a known peptoid and its shorter counterpart. Short brominated analogues displayed up to 32-fold increase of the activity against S. aureus and 16- to 64-fold against E. coli and P. aeruginosa alongside reduced cytotoxicity. The biological effect of halogens seems to be linked to the relative hydrophobicity and self-assembly properties of the compounds. By small angle X-ray scattering (SAXS) we have demontrated how the self-assembled structures are dependent on the size of the halogen, degree of substitution and length of the peptoid, and correlated these features to their activity.

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“…The biological studies showed that many of them exhibited more powerful inhibitory activities than the related α‐type natural product. In 2018, Paulsen et al developed a series of cyclic tetrapeptides containing one β 2 ‐amino acid in the sequence (Figure B). Low toxicity and high antimicrobial activity of these potent peptides suggested that the β 2 ‐amino acid containing scaffold was valuable for further design of novel antimicrobial agents.…”

Section: Strategies To Develop Cyclic Peptides Into Therapeutic Agentsmentioning

confidence: 99%

A gold mine for drug discovery: Strategies to develop cyclic peptides into therapies

Jing

Jin

2019

Medicinal Research Reviews

119

130

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As a versatile therapeutic modality, peptides attract much attention because of their great binding affinity, low toxicity, and the capability of targeting traditionally “undruggable” protein surfaces. However, the deficiency of cell permeability and metabolic stability always limits the success of in vitro bioactive peptides as drug candidates. Peptide macrocyclization is one of the most established strategies to overcome these limitations. Over the past decades, more than 40 cyclic peptide drugs have been clinically approved, the vast majority of which are derived from natural products. The de novo discovered cyclic peptides on the basis of rational design and in vitro evolution, have also enabled the binding with targets for which nature provides no solutions. The current review summarizes different classes of cyclic peptides with diverse biological activities, and presents an overview of various approaches to develop cyclic peptide‐based drug candidates, drawing upon series of examples to illustrate each strategy.

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An amphipathic cyclic tetrapeptide scaffold containing halogenated β^2,2‐amino acids with activity against multiresistant bacteria

Cited by 9 publications

References 25 publications

Natural and Synthetic Halogenated Amino Acids—Structural and Bioactive Features in Antimicrobial Peptides and Peptidomimetics

Natural and Synthetic Halogenated Amino Acids—Structural and Bioactive Features in Antimicrobial Peptides and Peptidomimetics

Halogenation as a tool to tune antimicrobial activity of peptoids

A gold mine for drug discovery: Strategies to develop cyclic peptides into therapies

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An amphipathic cyclic tetrapeptide scaffold containing halogenated β2,2‐amino acids with activity against multiresistant bacteria

Cited by 9 publications

References 25 publications

Natural and Synthetic Halogenated Amino Acids—Structural and Bioactive Features in Antimicrobial Peptides and Peptidomimetics

Natural and Synthetic Halogenated Amino Acids—Structural and Bioactive Features in Antimicrobial Peptides and Peptidomimetics

Halogenation as a tool to tune antimicrobial activity of peptoids

A gold mine for drug discovery: Strategies to develop cyclic peptides into therapies

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Product

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An amphipathic cyclic tetrapeptide scaffold containing halogenated β^2,2‐amino acids with activity against multiresistant bacteria