Unexpected dimerization of a tripeptide comprising a β,γ‐diamino acid

Wan, Yang; Baltaze, Jean‐Pierre; Kouklovsky, Cyrille; Miclet, Emeric; Alezra, Valérie

doi:10.1002/psc.3143

Cited by 4 publications

(3 citation statements)

References 38 publications

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“…Peptide design . Recently, one of our studies showed that β,γ‐DiAAs are capable of promoting dimerization when incorporated into α/γ‐hybrid tripeptides through extra hydrogen bonds [44] …”

Section: Resultsmentioning

confidence: 99%

“…Recently, one of our studies showed that β,γ-DiAAs are capable of promoting dimerization when incorporated into α/γ-hybrid tripeptides through extra hydrogen bonds. [44] We thereby questioned whether these short peptides could serve as β-strand mimics in cyclopeptides. Inspired by the GS sequence, we employed the β-turn inducer ' D Phe-Pro' to constrain the dimeric tripeptide at both ends ( Figure 2).…”

Section: Peptide Design and Synthesismentioning

confidence: 99%

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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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Section: Resultsmentioning

confidence: 99%

Section: Peptide Design and Synthesismentioning

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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“…These findings are reminiscent of our previous results that instead of intra-molecular interaction, inter-molecular H-bonds are formed when (βR,γR)-DiAA 3 is introduced into short peptides. [45] As can be found in Table 2, the 3 J CαH-NH coupling constants of the Leu, Orn and Val (ranging between 8.6 and 9.1 Hz) of GS corresponds to a β-sheet structure. [46] A set of comparable values were calculated in GS6 while not in other analogues, signifying an analogous secondary structure between GS6 and GS.…”

Section: Introductionmentioning

confidence: 91%

Development of Therapeutic Gramicidin S Analogues Bearing Plastic β,γ‐Diamino Acids

Guan

Chen

et al. 2020

ChemMedChem

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Gramicidin S (GS), one of the most widely investigated antimicrobial peptides (AMPs), is known for its robust antimicrobial activity. However, it is restricted to topical applications due to undesired hemolytic activity. With the aim to obtain non-toxic GS analogues, we describe herein a molecular approach where the native GS β-turn region is replaced by synthetic β,γ-diamino acids (β,γ-DiAAs). Four β,γ-DiAA diastereomers were employed to mimic β-turn structure to afford GS analogues GS3-6 that exhibit diminished hemolytic activity. A comparative structural study demonstrates that the (βR,γS)-DiAA displays the most stable β-turn mimic. To further improve the therapeutic index (e.g. high antibacterial activity and low hemolytic activity) and to extend the molecular diversity, GS5 and GS6 were used as structural scaffolds to introduce additional hydrophobic or hydrophilic groups. We show that GS6K, GS6F and GS display comparable antibacterial activity while GS6K and GS6F possess significantly decreased toxicity. Moreover, antibacterial mechanism studies suggest that GS6K kills bacteria mainly through the disruption of membrane. Results and DiscussionScope of Lead Peptide Molecular Design and Synthesis. Initially, four diastereomeric GS analogues (GS3-6, Figure 1) were synthesized to evaluate in both biological and conformational aspects. The β,γ-DiAAs were prepared using the synthetic strategy previously described by our group starting from α-amino acids. [42] With respect to the aromatic character in the β-turn region, [36,39] D-and L-phenylalanine were chosen as starting materials (Scheme 1). Cbz-protected intermediates 7, 8, 9 and 10 were prepared as previously described. [23,43] Since the configuration of an analogue of compound 9 has been previously determined by crystallographic structure, [43] the other compounds could thereby be differentiated by the comparison of their NMR spectrum with their enantiomers. Noteworthy, the separation of the diastereomers is rather difficult when directly applying the silica gel chromatography. Alternatively, the minor diastereomers (8 and 10) can be easily precipitated in the presence of cold diethyl ether, and it consequently allows the major diastereomers (7 and 9) being purified by chromatography. To allow the solid phase synthesis, Cbz protecting group was further transferred to Fmoc protecting group (Scheme 1).Previous studies have demonstrated that GS and its analogues can be readily synthesized by solution-phase cyclization of the corresponding linear precursor peptides with protected side chains. [44] To this end, the linear precursors were assembled by following an either conventional or microwave-assistant solid phase Fmoc/tBu strategy. All Fmoc-protected α-amino acids are commercially available. Each projected peptide was assembled stepwise on the solid support starting from Fmoc-Pro-2-Chlorotrityl Chloride (CTC) Resin. During the sequential coupling, HBTU/HOBt (conventional synthesis) or HBTU (microwave-assistant synthesis) was used for activation, DiPEA as base,...

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Photocatalytic carbocarboxylation of styrenes with CO₂for the synthesis of γ-aminobutyric esters

et al. 2021

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Unexpected dimerization of a tripeptide comprising a β,γ‐diamino acid

Cited by 4 publications

References 38 publications

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

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

Development of Therapeutic Gramicidin S Analogues Bearing Plastic β,γ‐Diamino Acids

Photocatalytic carbocarboxylation of styrenes with CO₂for the synthesis of γ-aminobutyric esters

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Unexpected dimerization of a tripeptide comprising a β,γ‐diamino acid

Cited by 4 publications

References 38 publications

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

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

Development of Therapeutic Gramicidin S Analogues Bearing Plastic β,γ‐Diamino Acids

Photocatalytic carbocarboxylation of styrenes with CO2for the synthesis of γ-aminobutyric esters

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Photocatalytic carbocarboxylation of styrenes with CO₂for the synthesis of γ-aminobutyric esters