The Effect of Backbone-Heteroatom Substitution on the Folding of Peptides - A Single Fluorine Substituent Prevents a?-Heptapeptide from Folding into a314-Helix (NMR Analysis)

Mathad, Raveendra I.; Gessier, François; Seebàch, Dieter; Jaun, Bernhard

doi:10.1002/hlca.200590008

Cited by 56 publications

(96 citation statements)

References 41 publications

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“…The exploitation of these effects in organic and biological chemistry is currently an emerging area [38–41]. Our experimental and theoretical work illustrates how these effects result in enhanced regiocontrol in the ring-opening chemistry of bicyclic aziridiniums, complementing much of the research to date on the stereoelectronic effects of fluorine, which mostly focuses on their stereochemical ramifications [42]. …”

Section: Resultsmentioning

confidence: 99%

Fluorine as a Regiocontrol Element in the Ring Opening of Bicyclic Aziridiniums

Lam

Houk²,

Cossy

et al. 2012

Helvetica Chimica Acta

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The origin of the variation in the regioselectivity of the nucleophilic ring-opening of a series of bicyclic aziridinium ions derived from N-alkylprolinols was investigated by quantum chemical computations (M06-2X/6-31+G(d,p)—SMD). These aziridiniums differ only in the degree and the stereochemistry of fluoro substitution at C(4). With the azide ion as nucleophile, the ratio of the piperidine to the pyrrolidine product was computed. An electrostatic gauche effect influences the conformation of the adjoining five-membered ring in the fluorinated bicyclic aziridinium. This controls the regioselectivity of the aziridinium ring-opening.

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Section: Resultsmentioning

confidence: 99%

Fluorine as a Regiocontrol Element in the Ring Opening of Bicyclic Aziridiniums

Lam

Houk²,

Cossy

et al. 2012

Helvetica Chimica Acta

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“…158 in a right-handed direction (a ''3.2-helix''). For steric reasons only H, OH, or F are allowed 8 in the axial positions (Figure 3), a methyl group is not. Thus, homologs of Aib (b 2 -and b 3 hAib, homoaminoisobutyric acid) are helix-breaking in the ''b-regime,'' 4 while Aib itself is strongly 3 10 -helix-inducing in the ''a-world.''…”

Section: 454749mentioning

confidence: 98%

Helices and other secondary structures of β‐ and γ‐peptides

Seebàch

Hook

Glättli³

2005

Biopolymers

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212

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The principal secondary structural motifs adopted by peptides assembled from beta-amino acid units are discussed: the 14-, 12-, 10-, 12/10-, and 8-helices, as well as the hairpin turn, extended structures, stacks, and sheets. Features that promote a particular folding propensity are outlined and illustrated by structures determined in solution (NMR) and in the solid-state (x-ray). The N-C(beta)-C(alpha)-CO dihedral angles from molecular dynamics simulations, which are indicative of a particular secondary structure, are presented. A brief description of a helix and a turn of gamma-peptides is also given.

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“…One interesting observation among this set of peptides is the difference in hemolytic activity between the epimeric 2-hydroxy peptides 14 and 15 [25]. The configuration of the stereogenic center bearing the OH group exerts a major influence on the structures of these two peptides; whereas 15 (of unlike-configuration) adopts a 3 14 -helix, the like-configured compound 14 exhibited no helical conformation (NMR investigation [43]). Likewise, peptide 11, which also contains a disubstituted b-amino acid of like-configuration, showed no helical NMR structure, with peptides 12 and 13 assuming the 3 14 -helix [43] [44].…”

mentioning

confidence: 97%

“…The configuration of the stereogenic center bearing the OH group exerts a major influence on the structures of these two peptides; whereas 15 (of unlike-configuration) adopts a 3 14 -helix, the like-configured compound 14 exhibited no helical conformation (NMR investigation [43]). Likewise, peptide 11, which also contains a disubstituted b-amino acid of like-configuration, showed no helical NMR structure, with peptides 12 and 13 assuming the 3 14 -helix [43] [44]. Such F-and OH-containing b-peptides have been used for studies aimed at understanding the proteolytic stability of b-peptides [25].…”

mentioning

confidence: 98%

Exploring the Antibacterial and Hemolytic Activity of Shorter‐ and Longer‐Chain β‐, α,β‐, and γ‐Peptides, and of β‐Peptides from β²‐3‐Aza‐ and β³‐2‐Methylidene‐amino Acids Bearing Proteinogenic Side Chains – A Survey

Arvidsson

Ryder²,

Weiss

et al. 2005

Chemistry & Biodiversity

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The antibacterial activities of 31 different beta-, mixed alpha/beta-, and gamma-peptides, as well as of beta-peptides derived from beta2-3-aza- and beta3-2-methylidene-amino acids were assayed against six pathogens (Enterococcus faecalis, Staphylococcus aureus, Streptococcus pneumoniae, Escherichia coli, Klebsiella pneumoniae, and Pseudomonas aeruginosa), and the results were compared with literature data. The interaction of these peptides with mammalian cells, as modeled by measuring the hemolysis of human erythrocytes, was also investigated. In addition to those peptides designed to fold into amphiphilic helical conformations with positive charges on one face of the helix, one new peptide with hemolytic activity was detected within the sample set. Moreover, it was demonstrated that neither cationic peptides used for membrane translocation (beta3-oligoarginines), nor mixed alpha/beta- or gamma-peptides with somatostatin-mimicking activities display unwanted hemolytic activity.

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The Effect of Backbone-Heteroatom Substitution on the Folding of Peptides - A Single Fluorine Substituent Prevents a?-Heptapeptide from Folding into a314-Helix (NMR Analysis)

Cited by 56 publications

References 41 publications

Fluorine as a Regiocontrol Element in the Ring Opening of Bicyclic Aziridiniums

Fluorine as a Regiocontrol Element in the Ring Opening of Bicyclic Aziridiniums

Helices and other secondary structures of β‐ and γ‐peptides

Exploring the Antibacterial and Hemolytic Activity of Shorter‐ and Longer‐Chain β‐, α,β‐, and γ‐Peptides, and of β‐Peptides from β²‐3‐Aza‐ and β³‐2‐Methylidene‐amino Acids Bearing Proteinogenic Side Chains – A Survey

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The Effect of Backbone-Heteroatom Substitution on the Folding of Peptides - A Single Fluorine Substituent Prevents a?-Heptapeptide from Folding into a314-Helix (NMR Analysis)

Cited by 56 publications

References 41 publications

Fluorine as a Regiocontrol Element in the Ring Opening of Bicyclic Aziridiniums

Fluorine as a Regiocontrol Element in the Ring Opening of Bicyclic Aziridiniums

Helices and other secondary structures of β‐ and γ‐peptides

Exploring the Antibacterial and Hemolytic Activity of Shorter‐ and Longer‐Chain β‐, α,β‐, and γ‐Peptides, and of β‐Peptides from β2‐3‐Aza‐ and β3‐2‐Methylidene‐amino Acids Bearing Proteinogenic Side Chains – A Survey

Contact Info

Product

Resources

About

Exploring the Antibacterial and Hemolytic Activity of Shorter‐ and Longer‐Chain β‐, α,β‐, and γ‐Peptides, and of β‐Peptides from β²‐3‐Aza‐ and β³‐2‐Methylidene‐amino Acids Bearing Proteinogenic Side Chains – A Survey