Exploring the Conformational and Biological Versatility of β‐Turn‐Modified Gramicidin S by Using Sugar Amino Acid Homologues that Vary in Ring Size

Knijnenburg, Annemiek D.; Tuin, Adriaan W.; Spalburg, Emile; Neeling, Albert J. de; Mars-Groenendijk, Roos H.; Noort, Daan; Otero, José M.; Llamas-Saíz, Antonio L.; Raaij, Mark J. van; Marel, Gijs A. van der; Overkleeft, Herman S.; Overhand, Mark

doi:10.1002/chem.201002895

Cited by 33 publications

(24 citation statements)

References 64 publications

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“…GS adopted a C 2 ‐symmetric antiparallel β‐sheet with two type II′ β‐turns at the d ‐Phe‐Pro sequences . Several GS analogs, which contained thioindolizines, indolizines, sugar amino acids and their homologs, d ‐Pro‐Phe, morpholine amino acids, or di‐γ‐peptide at the d ‐Phe‐Pro sequence, have been studied with the aim of designing potent antimicrobial agents …”

Section: Resultsmentioning

confidence: 99%

“…The GS B ‐Nip 2 derivative favored solvation by 13.95 kcal mol −1 in CH 2 Cl 2 and by 24.97 kcal mol −1 in water at the SMD M06‐2X/6–31G(d) level of theory compared with those of GS B . It was expected that the replacement of the d ‐Phe‐Pro sequence of GS by the ( R )‐Nip‐( S )‐Nip segment might make GS less hydrophobic and decrease the hemolytic activity, as suggested for GS derivatives containing sugar amino acids as a turn motif . However, further experiments are needed to evaluate the antimicrobial activity of the GS B ‐Nip 2 derivative.…”

Section: Resultsmentioning

confidence: 99%

“…However, further experiments are needed to evaluate the antimicrobial activity of the GS B ‐Nip 2 derivative. Based on measurements of the CD spectra of GS and its derivatives containing sugar amino acids in methanol and water, it has been suggested that GS adopts the same secondary structure in both solvents; in contrast, its derivatives exhibited an enhanced excitation that differed between water and methanol, indicating that the secondary structure was more pronounced in methanol . To estimate the relative conformational flexibilities of GS and the GS B ‐Nip 2 derivative, we compared the conformational entropies of these compounds in CH 2 Cl 2 and in water.…”

Section: Resultsmentioning

confidence: 99%

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Hairpin formation promoted by the heterochiral dinipecotic acid segment: A DFT study

Kang

Park

2015

Biopolymers

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Conformational preferences for the turn and β-hairpin structures of Ala-based peptides [Ac-Ala(n)-(R)-Nip-(S)-Nip-Ala(n)-X (n = 0-2; X = NHMe or NMe2)] containing nipecotic acid (Nip) residues were carried out using the density functional M06-2X and the implicit solvation model SMD in CH2Cl2 and/or water. The turn structure of the (R)-Nip-(S)-Nip segment with a C10 H-bond between two terminal groups was found to be most preferred (populated at 98.9%) in CH2Cl2; this structure is consistent with IR and (1)H NMR results. The stabilities of the β-hairpins containing the (R)-Nip-(S)-Nip segment as a turn motif relative to the extended structures increased with peptide sequence length. The relative strengths of the H-bonds between the carbonyl oxygen and the amide hydrogen appeared to be responsible for stabilizing the turn and β-hairpin structures in CH2Cl2. In addition, the (R)-Nip-(S)-Nip segment exhibited the capability to be incorporated into one of the two β-turn motifs of gramicidin S (GS). The structure of this GS derivative (GS-Nip2 ) was generally similar to the native peptide but was less hydrophobic and it is therefore expected to exhibit lower hemolytic activity; however, further experiments are needed to evaluate its antimicrobial activity. The structure of GS-Nip2 was somewhat more flexible than GS in solvents of higher polarity. Thus, our calculated results regarding the turn and β-hairpin motifs of the (R)-Nip-(S)-Nip segment indicate that this structure might be useful for the design of bioactive macrocyclic peptides containing β-hairpin mimics as well as binding epitopes in protein-protein and protein-nucleic acid recognitions.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Hairpin formation promoted by the heterochiral dinipecotic acid segment: A DFT study

Kang

Park

2015

Biopolymers

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“…GS adopts a C 2 ‐symmetric antiparallel β‐sheet with two type II′ β‐turns at the D ‐Phe‐Pro sequences 52–54. Several GS analogues, which contain thioindolizines, indolizines, sugar amino acids and their homologues, D ‐Pro‐Phe, or morpholine amino acids at the D ‐Phe‐Pro sequence, have been studied to design the potent antimicrobial agents 55–60. In the trigonal crystal of GS, there are one and a half crystallographically independent peptide molecules A and B (i.e., GS A and GS B ), of which the latter has the molecular C 2 symmetry axis 54…”

Section: Resultsmentioning

confidence: 99%

Computationally designed β‐turn foldamers of γ‐peptides based on 2‐(aminomethyl)cyclohexanecarboxylic acid

Kang

Byun

2012

Biopolymers

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The γ-peptide β-turn structures have been designed computationally by the combination of chirospecific γ(2),(3)-residues of 2-(aminomethyl)cyclohexanecarboxylic acid (γAmc(6)) with a cyclohexyl constraint on the C(α) -C(β) bond using density functional methods in water. The chirospecific γAmc(6) dipeptide with the (2S,3S)-(2R,3R) configurations forms a stable turn structure in water, resembling a type II' turn of α-peptides, which can be used as a β-turn motif in β-hairpins of Ala-based α-peptides. The γAmc(6) dipeptide with homochiral (2S,3S)-(2S,3S) configurations but different cyclohexyl puckerings shows the capability to be incorporated into one of two β-turn motifs of gramicidin S. The overall structure of this gramicidin S analogue is quite similar to the native gramicidin S with the same patterns and geometries of hydrogen bonds. Our calculated results and the recently observed results may imply the wider applicability of chirospecific γ-peptides with a cyclohexyl constraint on the backbone to form various peptide foldamers.

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“…Nowadays, SAAs are widely used in the design and synthesis of foldamers [2] as they have i) a versatile nature; ii) tunable properties in terms of ring size, stereochemistry, substituents, and conformation; iii) adjustable hydrophilic/hydrophobic character as a function of the free/protected nature of their OH groups. [3][4][5][6][7] A large number of cyclic SAAs based on αto ε-amino acid motifs have been described; these mainly have either furanoid or pyranoid rings. Homo-and heterooligomers built up from such building blocks using solid-phase peptide synthesis (SPPS) could form different secondary structural elements and designed backbone scaffolds, similar to those occurring in polypeptides and proteins, but with different dynamic properties.…”

Section: Introductionmentioning

confidence: 99%

Approaches to Pyranuronic β‐Sugar Amino Acid Building Blocks of Peptidosaccharide Foldamers

et al. 2018

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Pyranuronic β‐sugar amino acids (β‐SAAs) are biocompatible and tuneable building blocks of foldamers and chimera‐peptides. The scalable and economical total synthesis of two building blocks is described here. These C‐4 epimers, Fmoc‐GlcAPU(Me)‐OH (7) and Fmoc‐GalAPU(Me)‐OH (8), which are suitable for solid phase peptide synthesis, were prepared via a common oxime intermediate 16. The new synthesis uses nine consecutive steps, starting from methyl α‐d‐glucopyranoside (6). The synthesis is fine‐tuned, optimized, and ready for large‐scale and cost‐efficient production.

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Exploring the Conformational and Biological Versatility of β‐Turn‐Modified Gramicidin S by Using Sugar Amino Acid Homologues that Vary in Ring Size

Cited by 33 publications

References 64 publications

Hairpin formation promoted by the heterochiral dinipecotic acid segment: A DFT study

Hairpin formation promoted by the heterochiral dinipecotic acid segment: A DFT study

Computationally designed β‐turn foldamers of γ‐peptides based on 2‐(aminomethyl)cyclohexanecarboxylic acid

Approaches to Pyranuronic β‐Sugar Amino Acid Building Blocks of Peptidosaccharide Foldamers

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