Solid-Phase Synthesis of Head to Side-Chain Tyr-Cyclodepsipeptides Through a Cyclative Cleavage From Fmoc-MeDbz/MeNbz-resins

Acosta, Gerardo; Murray, Laura; Royo, Míriam; Torre, Beatriz G. de la; Alberício, Fernando

doi:10.3389/fchem.2020.00298

Cited by 7 publications

(6 citation statements)

References 50 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Based on our previous work on synthesis of C-terminal modified peptides , and acylation strategies for amide activation that are limited to C-terminal modification, − we hypothesized that the amide bond next to Ser/Thr or Cys could be weakened by the N-functionalization with the respective side chains of these residues through carbonyl or thiocarbonyl insertion (Figure a). The resulting oxazolidinone or thiazolidinone cyclic moiety will weaken the amide bond by introducing a twist that distorts the pi-pi overlap of the C–N bond. , Interception of these intermediates with primary/secondary amines and alcohols would furnish the desired transamidated and esterified products (Figure a).…”

mentioning

confidence: 99%

Metal-Free Selective Modification of Secondary Amides: Application in Late-Stage Diversification of Peptides

et al. 2021

View full text Add to dashboard Cite

Here we solve a long-standing challenge of the siteselective modification of secondary amides and present a simple twostep, metal-free approach to selectively modify a particular secondary amide in molecules containing multiple primary and secondary amides. Density functional theory (DFT) provides insight into the activation of C−N bonds. This study encompasses distinct chemical advances for late-stage modification of peptides thus harnessing the amides for the incorporation of various functional groups into natural and synthetic molecules.

show abstract

mentioning

confidence: 99%

Metal-Free Selective Modification of Secondary Amides: Application in Late-Stage Diversification of Peptides

et al. 2021

View full text Add to dashboard Cite

show abstract

“…It has been utilized in the synthesis of cysteine-rich proteins, such as the cyclotides Kalata B1 and MCoTI-II, through a single cyclization/folding step within the ligation/folding buffer [40]. Furthermore, the MeDbz linker has been used for the on-resin cyclization of side-chain (SH of Cys, NH 2 of Dab, OH of Tyr)-to-tail cyclic peptides [80][81][82] and for the preparation of C-terminal modified peptides [83,84]. This concept of using unsymmetrical diamino benzoic resin has been further described by other groups who utilize different protecting groups for the second amine function [75,85,86].…”

Section: Diamino Benzoic Acid (Dbz)-benzimidazolinone (Cyclic Urea)mentioning

confidence: 99%

Safety-Catch Linkers for Solid-Phase Peptide Synthesis

Noki,

de la Torre,

Albericio

2024

Molecules

Self Cite

View full text Add to dashboard Cite

Solid-phase peptide synthesis (SPPS) is the preferred strategy for synthesizing most peptides for research purposes and on a multi-kilogram scale. One key to the success of SPPS is the continual evolution and improvement of the original method proposed by Merrifield. Over the years, this approach has been enhanced with the introduction of new solid supports, protecting groups for amino acids, coupling reagents, and other tools. One of these improvements is the use of the so-called “safety-catch” linkers/resins. The linker is understood as the moiety that links the peptide to the solid support and protects the C-terminal carboxylic group. The “safety-catch” concept relies on linkers that are totally stable under the conditions needed for both α-amino and side-chain deprotection that, at the end of synthesis, can be made labile to one of those conditions by a simple chemical reaction (e.g., an alkylation). This unique characteristic enables the simultaneous use of two primary protecting strategies: tert-butoxycarbonyl (Boc) and fluorenylmethoxycarbonyl (Fmoc). Ultimately, at the end of synthesis, either acids (which are incompatible with Boc) or bases (which are incompatible with Fmoc) can be employed to cleave the peptide from the resin. This review focuses on the most significant “safety-catch” linkers.

show abstract

“…35 Besides CPS, the Nbz/MeNbz and Bt linkers have found other important applications, enabling the access to posttranslational modications at the C-terminal peptide side of high structural and biomedical relevance, including C-terminal peptide esters and N-alkylamides and [36][37][38] head-to-tail and side chain-to-tail cyclic peptides. [39][40][41] From a synthetic point of view, it would be very attractive to use a single 1,2-diaminobenzene-type moiety for the preparation of peptides featuring C-terminal Nbz and Bt-type functionalities that combines the advantages of Dbz-COOH and MeDbz-COOH. Here, we show that C-terminal peptides amidated with 1,2-diaminobenzene (Dbz) can be efficiently converted in peptide-Nbz or peptide-Bt derivatives from the same initial peptide-Dbz-PAL-resin (PAL ¼ 4-(4-(aminomethyl)-3,5dimethoxyphenoxy)butanoic/pentanoic acid) precursor.…”

Section: Introductionmentioning

confidence: 99%

“…Besides CPS, the Nbz/MeNbz and Bt linkers have found other important applications, enabling the access to posttranslational modifications at the C-terminal peptide side of high structural and biomedical relevance, including C-terminal peptide esters and N -alkylamides and 36–38 head-to-tail and side chain-to-tail cyclic peptides. 39–41…”

Section: Introductionmentioning

confidence: 99%