Your search keyword '"Iteng Ng-Choi"' showing total 7 results

1. Solid-Phase Synthesis of Biaryl Cyclic Lipopeptides Derived from Arylomycins

Author

Iteng Ng-Choi, Eduard Figueras, Àngel Oliveras, Lidia Feliu, and Marta Planas

Subjects

Chemistry, QD1-999

Published

2020

2. Solid-phase synthesis of biaryl bicyclic peptides containing a 3-aryltyrosine or a 4-arylphenylalanine moiety

Author

Iteng Ng-Choi, Àngel Oliveras, Lidia Feliu, and Marta Planas

Subjects

borylation, cross-coupling, cyclization, macrocycles, solid-phase synthesis, Science, Organic chemistry, QD241-441

Abstract

A methodology for the solid-phase synthesis of biaryl bicyclic peptides containing a Phe-Phe, a Phe-Tyr or a Tyr-Tyr motif has been devised. This approach comprises two key steps. The first one involves the cyclization of a linear peptidyl resin containing the corresponding halo- and boronoamino acids via a microwave-assisted Suzuki–Miyaura cross coupling. This step is followed by the macrolactamization of the resulting biaryl monocyclic peptidyl resin leading to the formation of the expected biaryl bicyclic peptide. This study provides the first solid-phase synthesis of this type of bicyclic compounds being amenable to prepare a diversity of synthetic or natural biaryl bicyclic peptides.

Published

2019

3. Multivalent display of the antimicrobial peptides BP100 and BP143

Author

Imma Güell, Rafael Ferre, Kasper K. Sørensen, Esther Badosa, Iteng Ng-Choi, Emilio Montesinos, Eduard Bardají, Lidia Feliu, Knud J. Jensen, and Marta Planas

Subjects

antimicrobial activity, carbopeptides, multimeric structures, oxime ligation, phytopathogenic bacteria, Science, Organic chemistry, QD241-441

Abstract

Carbohydrates are considered as promising templates for the display of multiple copies of antimicrobial peptides. Herein, we describe the design and synthesis of chimeric structures containing two or four copies of the antimicrobial peptides KKLFKKILKYL-NH2 (BP100) and KKLfKKILKYL-NH2 (BP143) attached to the carbohydrate template cyclodithioerythritol (cDTE) or α-D-galactopyranoside (Galp). The synthesis involved the preparation of the corresponding peptide aldehyde followed by coupling to an aminooxy-functionalized carbohydrate template. After purification, the multivalent display systems were obtained in high purities (90–98%) and in good yields (42–64%). These compounds were tested against plant and human pathogenic bacteria and screened for their cytotoxicity on eukaryotic cells. They showed lower MIC values than the parent peptides against the bacteria analyzed. In particular, the carbopeptides derived from cDTE and Galp, which contained two or four copies of BP100, respectively, were 2- to 8-fold more active than the monomeric peptide against the phytopathogenic bacteria. These results suggest that preassembling antimicrobial peptides to multimeric structures is not always associated with a significant improvement of the activity. In contrast, the carbopeptides synthesized were active against human red blood cells pointing out that peptide preassembly is critical for the hemolytic activity. Notably, peptide preassembly resulted in an enhanced bactericidal effect.

Published

2012

4. Solid-phase synthesis of biaryl cyclic peptides containing a histidine-tyrosine linkage

Author

Lidia Feliu, Marta Planas, Àngel Oliveras, Iteng Ng-Choi, and Ministerio de Ciencia e Innovación (Espanya)

Subjects

Peptide antibiotics, chemistry.chemical_classification, Histidine residue, Bicyclic molecule, 010405 organic chemistry, Chemistry, Stereochemistry, Organic Chemistry, Antibiòtics pèptids, Peptides -- Synthesis, 010402 general chemistry, Ring (chemistry), 01 natural sciences, Biochemistry, Cyclic peptide, 0104 chemical sciences, Amino acid, Solid-phase synthesis, Drug Discovery, Tyrosine, Pèptids -- Síntesi, Histidine

Abstract

A solid-phase strategy for the synthesis of biaryl cyclic peptides containing a side-chain to side-chain His-Tyr linkage was developed. The key step was the macrocyclization of a linear peptidyl resin incorporating a 5-bromohistidine and a 3-boronotyrosine via the formation of the biaryl bond by means of a microwave-assisted Suzuki-Miyaura reaction. This method allowed direct access to biaryl cyclic peptides containing a 3- or 5-amino acid ring and bearing the histidine residue at the N- or the C-terminus, being especially conducive for analogues in which this amino acid is located at the C-terminus. This study also served to establish a strategy for the synthesis of biaryl cyclic peptides derived from the two hemispheres of the natural biaryl bicyclic peptides aciculitins Àngel Oliveras was recipient of predoctoral fellowship from the University of Girona. This work was supported by grants AGL2009-13255-C02-02/AGR, AGL2012-39880-C02-02, AGL2015-69876-C2-2-R (MINECO/FEDER, EU) and MPCUdG2016/038

Published

2019

5. Solid-Phase Synthesis of Biaryl Cyclic Lipopeptides Derived from Arylomycins

Author

Marta Planas, Àngel Oliveras, Lidia Feliu, Eduard Figueras, Iteng Ng-Choi, Agencia Estatal de Investigación, Ministerio de Economía y Competitividad (Espanya), and Ministerio de Ciencia e Innovación (Espanya)

Subjects

Chemistry, Solid-phase synthesis, General Chemical Engineering, Pèptids, General Chemistry, Peptides, QD1-999, Combinatorial chemistry, Síntesi en fase sólida, Article

Abstract

An efficient approach for the solid-phase synthesis of N-methylated tailed biaryl cyclic lipopeptides based on the structure of arylomycins was established. Each of these analogues incorporates an N-terminal linear lipopeptide attached to a biaryl cyclic tripeptide containing a Phe−Tyr, a Tyr−Tyr, or a His−Tyr linkage. This methodology first involved an intramolecular Suzuki−Miyaura arylation of a linear peptidyl resin incorporating the corresponding halogenated amino acid at the N-terminus and a boronotyrosine at the C-terminus. After N-methylation of the resulting biaryl cyclic peptidyl resin, the N-methylated lipopeptidyl tail was then assembled. The biaryl cyclic lipopeptides were purified and characterized This work was supported by Grants AGL2009-13255-C02-02/AGR, AGL2012-39880-C02-02/AGR, MPCUdG2016/038, and RTI2018-099410-B-C22 (MCIU/ AEI/FEDER, EU)

Published

2020

6. Solid-phase synthesis of biaryl cyclic peptides containing a histidine-phenylalanine linkage

Author

Marta Planas, Iteng Ng-Choi, Àngel Oliveras, Lidia Feliu, and Ministerio de Ciencia e Innovación (Espanya)

Subjects

Ciclització (Química), Stereochemistry, Bioengineering, Phenylalanine, 01 natural sciences, Biochemistry, Analytical Chemistry, Ring formation (Chemistry), Residue (chemistry), chemistry.chemical_compound, Solid-phase synthesis, Drug Discovery, Imidazole, Phenyl group, Histidine, chemistry.chemical_classification, Peptide antibiotics, 010405 organic chemistry, Chemistry, Antibiòtics pèptids, Peptides -- Synthesis, Cyclic peptide, 0104 chemical sciences, Intramolecular force, Molecular Medicine, Pèptids -- Síntesi

Abstract

The feasibility of the solid-phase intramolecular 4(5)-arylation of a histidine residue to obtain biaryl cyclic peptides bearing a His-Phe linkage was established. The synthetic strategy involved the preparation of a linear peptidyl resin incorporating a 5-bromohistidine and a 4-boronophenylalanine, and its cyclization through the formation of the biaryl bond between the imidazole of histidine and the phenyl group of phenylalanine via a microwave-assisted Suzuki-Miyaura cross-coupling. This methodology was applied to the preparation of biaryl cyclic peptides consisting of a 3- or 5-residue ring, incorporating the His residue at the N- or the C-terminus and bearing a Leu-Leu spacer or a -NH2 group at the C-terminus. In the case of the 3-residue ring peptides, the position of the His did not influence the macrocyclization. In contrast, to obtain the 5-member ring biaryl cyclic peptides, the His residue should be located at the N-terminus. It was also observed that the Leu-Leu spacer is crucial for the intramolecular arylation. These results suggest that this approach could be useful for the preparation of a diversity of synthetic and natural biaryl cyclic peptides bearing a His-Phe linkage Iteng Ng Choi was recipient of a predoctoral fellowship from the MICINN of Spain. Àngel Oliveras was recipient of predoctoral fellowship from the University of Girona. This work was supported by grants AGL2009-13255-C02-02/AGR, AGL2012-39880-C02-02, AGL2015-69876-C2-2-R (MINECO/FEDER, EU) and MPCUdG2016/038

Published

2020

7. Multivalent display of the antimicrobial peptides BP100 and BP143

Author

Emilio Montesinos, Marta Planas, Rafael Ferre, Esther Badosa, Lidia Feliu, Imma Güell, Iteng Ng-Choi, Kasper K. Sørensen, Eduard Bardají, and Knud J. Jensen

Subjects

Antimicrobial peptides, Peptide, medicine.disease_cause, phytopathogenic bacteria, Full Research Paper, lcsh:QD241-441, chemistry.chemical_compound, lcsh:Organic chemistry, medicine, Cytotoxicity, carbopeptides, lcsh:Science, chemistry.chemical_classification, Peptide antibiotics, antimicrobial activity, biology, GalP, Organic Chemistry, Antibiòtics pèptids, Peptides -- Synthesis, Pathogenic bacteria, Carbohydrate, biology.organism_classification, Combinatorial chemistry, Chemistry, Monomer, chemistry, Biochemistry, oxime ligation, biology.protein, multimeric structures, lcsh:Q, Pèptids -- Síntesi, Bacteria

Abstract

Carbohydrates are considered as promising templates for the display of multiple copies of antimicrobial peptides. Herein, we describe the design and synthesis of chimeric structures containing two or four copies of the antimicrobial peptides KKLFKKILKYL-NH2 (BP100) and KKLfKKILKYL-NH2 (BP143) attached to the carbohydrate template cyclodithioerythritol (cDTE) or α-D-galactopyranoside (Galp). The synthesis involved the preparation of the corresponding peptide aldehyde followed by coupling to an aminooxy-functionalized carbohydrate template. After purification, the multivalent display systems were obtained in high purities (90–98%) and in good yields (42–64%). These compounds were tested against plant and human pathogenic bacteria and screened for their cytotoxicity on eukaryotic cells. They showed lower MIC values than the parent peptides against the bacteria analyzed. In particular, the carbopeptides derived from cDTE and Galp, which contained two or four copies of BP100, respectively, were 2- to 8-fold more active than the monomeric peptide against the phytopathogenic bacteria. These results suggest that preassembling antimicrobial peptides to multimeric structures is not always associated with a significant improvement of the activity. In contrast, the carbopeptides synthesized were active against human red blood cells pointing out that peptide preassembly is critical for the hemolytic activity. Notably, peptide preassembly resulted in an enhanced bactericidal effect.

Published

2013