2020
DOI: 10.1039/c9ob02654a
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Introducing sequential aza-amino acids units induces repeated β-turns and helical conformations in peptides

Abstract: A major current issue in medicinal chemistry is the design of small peptide analogues resistant to proteolysis and able to adopt preferential conformations, while preserving the selectivity and efficiency of natural peptides.

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Cited by 10 publications
(22 citation statements)
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“…2), serving as a reference with respect to our previously published work. 23 Different NMR parameters were analysed to assess the hydrogen bonding and folding propensities of diaza-tripeptides, in particular the temperature dependency of the amide proton chemical shift (temperature coefficient Δ δ HN /Δ T ) and the through-space dipolar 1 H– 1 H ROE correlations.…”
Section: Resultsmentioning
confidence: 99%
“…2), serving as a reference with respect to our previously published work. 23 Different NMR parameters were analysed to assess the hydrogen bonding and folding propensities of diaza-tripeptides, in particular the temperature dependency of the amide proton chemical shift (temperature coefficient Δ δ HN /Δ T ) and the through-space dipolar 1 H– 1 H ROE correlations.…”
Section: Resultsmentioning
confidence: 99%
“…Finally, one α/aza/aza/pseudotripeptide, Phe-azaLys-azaVal-COCH 3 (abbreviated as FaLaV-COCH 3 ) mimicking the C -terminal arm FLV of 8 , was inserted in compounds 13 and 14 and evaluated alone (compound 15 ). The introduction of one aza-amino acid in peptides has shown significant success in providing biologically active peptides (see the references cited in Tonali et al, 2020 ). However, to our knowledge, only scarce examples of biologically active peptide mimics having two consecutive aza-amino acids have been reported ( Gante et al, 1995 ; Han et al, 1998 ).…”
Section: Resultsmentioning
confidence: 99%
“…These findings highlight the fact that the design of TTR-derived anti-Aβ agents requires a correct balance between advantages and disadvantages of using a protein versus peptide as therapeutic, and a compromise between efficacy, specificity, stability and conformational behavior is demanding. This consideration opens the way to the use of peptidomimetic foldamers, for example, as a new approach which might resolve a major issue in the use of peptides as drugs, by stabilizing secondary conformations similar to natural peptides and retaining the selectivity due to the lateral chains [156].…”
Section: Ttr-aβ Interaction-based Strategies To Design Anti-aβ Agentsmentioning
confidence: 99%