Synthesis of Cyclic Tetrapeptides via Ligation of Peptide Hydrazides

Tang, Shan; Zheng, Ji‐Min; Yang, Ke; Liu, Lei

doi:10.6023/a12040166

Cited by 21 publications

(13 citation statements)

References 11 publications

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“…Zhang and Tam proposed that the absence of oligomerization at higher concentrations resulted from the ring-chain tautomeric equilibrium of the transthioesterification step between the thioester and the thiol on N-terminal Cys. This observation was consistent with a recent study by Liu and co-workers on the synthesis of highly strained cyclic tetrapeptides by NCL . In Liu’s work, they found that cyclic monomers were formed exclusively at a concentration up to 1 mM and that significant cyclic dimer formation occurred at a concentration of 3 mM.…”

Section: Chemoselective Ligation-mediated Peptide Cyclization Creatin...mentioning

confidence: 99%

Ligation Technologies for the Synthesis of Cyclic Peptides

et al. 2019

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Cyclic peptides have been attracting a lot of attention in recent decades, especially in the area of drug discovery, as more and more naturally occurring cyclic peptides with diverse biological activities have been discovered. Chemical synthesis of cyclic peptides is essential when studying their structure−activity relationships. Conventional peptide cyclization methods via direct coupling have inherent limitations, like the susceptibility to epimerization at the C-terminus, poor solubility of fully protected peptide precursors, and low yield caused by oligomerization. In this regard, chemoselective ligation-mediated cyclization methods have emerged as effective strategies for cyclic peptide synthesis. The toolbox for cyclic peptide synthesis has been expanded substantially in the past two decades, allowing more efficient synthesis of cyclic peptides with various scaffolds and modifications. This Review will explore different chemoselective ligation technologies used for cyclic peptide synthesis that generate both native and unnatural peptide linkages. The practical issues and limitations of different methods will be discussed. The advance in cyclic peptide synthesis will benefit the biological and medicinal study of cyclic peptides, an important class of macrocycles with potentials in numerous fields, notably in therapeutics. CONTENTS

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Section: Chemoselective Ligation-mediated Peptide Cyclization Creatin...mentioning

confidence: 99%

Ligation Technologies for the Synthesis of Cyclic Peptides

et al. 2019

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“…Natural charge: The atom natural charge of compounds are given in Table-3. These data show that, the negative charge is mainly concentrated in the C(1) of pyrimidine ring, N(2), N (5) and N(6) of triazine ring, and C(7), C(8), C (11) and C(12) of benzene ring. These atoms make the electronegative area, they could combine with positive area of receptor.…”

Section: Quantitative Structure-activity Relationships Of the Trisubsmentioning

confidence: 82%

“…For pesticide molecules, too low-E LUMO or too high-E HOMO means that the molecule itself activity is too strong, it is easy to be metabolized in organism. The effect of pesticide is difficult to control, so the E LUMO or E HOMO of the pesticide molecule should be suitable to estimate expected value [10][11][12] .…”

Section: Quantitative Structure-activity Relationships Of the Trisubsmentioning

confidence: 99%

Quantitative Structure-Activity Relationships of the Trisubstitued Triazines Bearing Aminopyrimidine Group

Bi¹,

Hu²,

Chai³

et al. 2013

Asian J. Chem.

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The quantum study of the trisubstitued triazines bearing aminopyrimidine group was calculated by Gaussian 03 program. The energies, main composition and proportion of the frontier orbitals and electron density were analyzed. The study found that there exists correlation between the antibacterial activity of the trisubstitued triazines bearing aminopyrimidine group and energy. It was found that the C(3) and C(4) atoms were the active sites. In order to get the regression equation, the correlation analysis was done between some characteristic parameters of the compound and the experiental parameters of antimicrobial activity and good parameters were selected for the linear regression. The result shows that the total energy of compound (Etot), molecular weight (M), hydrophobic parameter (log P) are the main influencing factors for the antibacterial activity of the compound and when the log P is in the 0~3.881 interval.

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“…Thus, four cyclic tetrapeptides containing all L-amino acids cyclo(L-Cys-L-Leu-L-Ala-L-Leu), cyclo(L-Cys-L-His-L-Gly-L-Trp), cyclo(L-Cys-L-Val-L-Gly-L-Ile) and cyclo(L-Cys-L-His-L-Trp-L-Gly) have been successfully prepared in moderate yields (∼40%) through intramolecular native chemical ligation (NCL) (Scheme 6). 56,57 Fmoc-SPPS on a hydrazine 2-chlorotrityl resin (26) was used to prepare the peptide hydrazide (27) and its conversion to acyl azide (28) in solution followed. The peptide hydrazide was used as a precursor to the corresponding peptide thioester (29), which undergo NCL (30) to afford the corresponding cyclotetrapeptide (31).…”

Section: Ring Contraction Strategiesmentioning

confidence: 99%

An update on new methods to synthesize cyclotetrapeptides

2015

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Cyclotetrapeptides are important bioactive lead drug molecules that display a wide spectrum of pharmacological activities. However, the synthesis of cyclotetrapeptides from their linear precursors is challenging due to the highly constrained conformation required for cyclisation, thus hampering their progress to a clinical setting. This review provides an account of the reported methods used for the synthesis of cyclotetrapeptides.

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Synthesis of Cyclic Tetrapeptides via Ligation of Peptide Hydrazides

Cited by 21 publications

References 11 publications

Ligation Technologies for the Synthesis of Cyclic Peptides

Ligation Technologies for the Synthesis of Cyclic Peptides

Quantitative Structure-Activity Relationships of the Trisubstitued Triazines Bearing Aminopyrimidine Group

An update on new methods to synthesize cyclotetrapeptides

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