Toward solid-phase peptide fragment ligation by a traceless-Ugi multicomponent reaction approach

Jobin, Steve; Méjean, Alexia; Galindo, Sindy-Marcela; Liang, Xinxia; Vézina‐Dawod, Simon; Biron, Éric

doi:10.1039/c6ob02342h

Cited by 9 publications

(7 citation statements)

References 50 publications

(66 reference statements)

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“…Lower conversion rates and yields were observed with shorter reaction times (entries 1 and 2). MW irradiations have been shown to accelerate and improve Ugi-4CR 33,51,52,67,68 but in our case no significant improvement was observed after 1 or 2 h of MW heating at 60°C (entries 4 and 5). For this reason and based on the possibility to perform parallel synthesis more efficiently, the room temperature condition was selected to conduct the next experiments.…”

Section: Resultscontrasting

confidence: 60%

Convenient two-step synthesis of highly functionalized benzo-fused 1,4-diazepin-3-ones and 1,5-diazocin-4-ones by sequential Ugi and intramolecular S N Ar reactions

et al. 2017

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Benzodiazepinones are an important family of heterocycles with very attractive pharmacological properties and peptidomimetic abilities. We report herein a rapid and efficient two-step synthesis of polysubstituted 1,4-benzodiazepin-3-ones and 1,5-benzodiazocin-4-ones using a multicomponent condensation/cyclization strategy. The approach uses an Ugi four-component reaction to condense readily available N α-Fmoc-amino acids, amines and isocyanides with a 2fluorobenzaldehyde derivative followed by a one-pot Fmoc-group removal, intramolecular aromatic nucleophilic substitution for ring closure and side chain deprotection. The described method gives access to benzo-fused 7-and 8-membered rings bearing a wide variety of functionalized substituents and was applied to efficiently prepare tri-and tetrasubstituted 1,4benzodiazepin-3-ones and 1,5-benzodiazocin-4-ones in high yields in two straightforward steps.

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Section: Resultscontrasting

confidence: 60%

Convenient two-step synthesis of highly functionalized benzo-fused 1,4-diazepin-3-ones and 1,5-diazocin-4-ones by sequential Ugi and intramolecular S N Ar reactions

et al. 2017

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“…Thus, we aimed at finding out whether the turn-inducing capacity of the N-alkylated peptidomimetic fragment is sufficient to fold the peptides into parallel b-sheets without the positive influence of the Thorpe-Ingold effect provided by the geminal methyl substituents. The versatility of the MCR method also enabled the facile synthesis of the non-N-alkylated b-sheet, peptide 8, using the acid-labile 2,4-dimethoxyphenyl substituent [17] (arising from the aldehyde component), which allows the cleavage at that specific position. Scheme 2 B (upper panel) shows a comparison of the circular dichroism (CD) spectra in acetate buffer (AcB) of the N-alkylated peptides 5 a, 6 a, and 7 a with the non-N-alkylated one (8), all based on the DADME residue.…”

Section: Angewandte Chemiementioning

confidence: 99%

Improved Stability and Tunable Functionalization of Parallel β‐Sheets via Multicomponent N‐Alkylation of the Turn Moiety

et al. 2019

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In contrast to the myriad of methods available to produce α‐helices and antiparallel β‐sheets in synthetic peptides, just a few are known for the construction of stable, non‐cyclic parallel β‐sheets. Herein, we report an efficient on‐resin approach for the assembly of parallel β‐sheet peptides in which the N‐alkylated turn moiety enhances the stability and gives access to a variety of functionalizations without modifying the parallel strands. The key synthetic step of this strategy is the multicomponent construction of an N‐alkylated turn using the Ugi reaction on varied isocyano‐resins. This four‐component process assembles the orthogonally protected turn fragment and incorporates handles serving for labeling/conjugation purposes or for reducing peptide aggregation. NMR and circular dichroism analyses confirm the better‐structured and more stable parallel β‐sheets in the N‐alkylated peptides compared to the non‐functionalized variants.

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“…Our strategy was based on a traceless‐Ugi multicomponent reaction we have recently described to efficiently couple peptide fragments on solid support (Figure a) . Because it involves the reaction of isocyanide, carboxylic acid, amine and carbonyl compounds to afford a α‐acylamino amide, the Ugi four‐component reaction (Ugi‐4CR) is a very attractive approach to form N ‐substituted peptide bonds and perform one‐pot backbone anchoring.…”

Section: Introductionmentioning

confidence: 99%

“…Because it involves the reaction of isocyanide, carboxylic acid, amine and carbonyl compounds to afford a α‐acylamino amide, the Ugi four‐component reaction (Ugi‐4CR) is a very attractive approach to form N ‐substituted peptide bonds and perform one‐pot backbone anchoring. In this previous study, an on‐resin Ugi‐4CR was used to attach a carboxyl free peptide to a supported peptide bearing a free N‐terminal amine via the formation of an N‐protected amide bond at the ligation site . Afterward, the generated backbone amide protecting group was efficiently removed by microwave‐assisted acidolysis with trifluoroacetic acid (TFA) to afford a fully deprotected peptide.…”

Section: Introductionmentioning

confidence: 99%

Development of a solid‐phase traceless‐Ugi multicomponent reaction for backbone anchoring and cyclic peptide synthesis

2018

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A new one‐pot methodology to anchor peptides by their backbone to a solid support using an isocyanide‐based multicomponent reaction is described. The approach uses a microwave‐assisted Ugi four‐component reaction to simultaneously condense and bind an N‐protected amino acid and an amino ester to a supported aldehyde. Afterward, the generated backbone anchored dipeptide can be used in solid‐phase peptide synthesis to prepare head‐to‐tail cyclic peptides. Moreover, we also show that peptide fragment ligation can be performed with the described one‐pot anchoring. The backbone anchored peptides can be efficiently released from the resin by microwave‐assisted acidolysis with trifluoroacetic acid. This straightforward one‐pot anchoring approach was also applied to condense fragments and prepare a variety of linear and macrocyclic peptides.

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Toward solid-phase peptide fragment ligation by a traceless-Ugi multicomponent reaction approach

Cited by 9 publications

References 50 publications

Convenient two-step synthesis of highly functionalized benzo-fused 1,4-diazepin-3-ones and 1,5-diazocin-4-ones by sequential Ugi and intramolecular S N Ar reactions

Convenient two-step synthesis of highly functionalized benzo-fused 1,4-diazepin-3-ones and 1,5-diazocin-4-ones by sequential Ugi and intramolecular S N Ar reactions

Improved Stability and Tunable Functionalization of Parallel β‐Sheets via Multicomponent N‐Alkylation of the Turn Moiety

Development of a solid‐phase traceless‐Ugi multicomponent reaction for backbone anchoring and cyclic peptide synthesis

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