Molecular construction of HIV-gp120 discontinuous epitope mimics by assembly of cyclic peptides on an orthogonal alkyne functionalized TAC-scaffold

Werkhoven, Paul R.; Elwakiel, M.; Meuleman, Theodorus J.; Ufford, H. C. Quarles van; Kruijtzer, John A. W.; Liskamp, Rob M. J.

doi:10.1039/c5ob02014j

Cited by 16 publications

(17 citation statements)

References 22 publications

(34 reference statements)

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“…Therefore, the serum stability of cateslytin (1) and the most potent peptide synlytin (7) was determined by a method used previously in our group. 38 Human serum was used to evaluate the stability of the peptides for up to 24h at 37 °C (Figure 1). …”

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confidence: 99%

Highly potent antimicrobial peptide derivatives of bovine cateslytin

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Liskamp

2016

RSC Adv.

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confidence: 99%

Highly potent antimicrobial peptide derivatives of bovine cateslytin

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Liskamp

2016

RSC Adv.

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“…Next, these azide‐containing hinges 17 and 18 were used in the cyclization of a peptide containing C‐ and N‐terminal cysteine residues. It was decided to use a peptide sequence corresponding to one of the three loops present in the HIV‐gp120 discontinuous epitope interaction with CD4 (peptide 19 , CLTRDGGKC, cysteine residues are underlined), which in the past gave considerable solubility problems when cyclized with the original aromatic dibromide hinge 4 , leading to N 3 ‐DBMB‐gp120 ( 22 ) . Both hinges 17 and 18 reacted cleanly and quickly with the crude linear peptide to form the cyclized peptides N 3 ‐TADB‐gp120 ( 20 ) and N 3 ‐DBMT‐gp120 ( 21 ) in good overall yields of 26 % for cyclic peptide 20 and 28 % for cyclic peptide 21 (Figure ).…”

Section: Resultsmentioning

confidence: 99%

“…gp120 (19) : The peptide was synthesized according to the protocol described above on a 0.25 mmol scale. This gave crude peptide 19 (269.8 mg), which was used without any purification in the cyclization step.…”

Section: Methodsmentioning

confidence: 99%

“…N 3 ‐DBMB‐gp120 (22) : Crude gp120 ( 19 , 48.8 mg, 40 μmol, 1 equiv) was treated with the previously described azido benzylic dibromide hinge 4 (12.8 mg, 40 μmol, 1 equiv) according to the cyclization method described above. The resulting crude cyclic peptide was dissolved in DMSO (500 μL), HPLC buffer B (2.5 mL) and HPLC buffer A (2 mL) and subjected to purification by preparative HPLC.…”

Section: Methodsmentioning

confidence: 99%

“…In the past we used a derivative of benzylic tribromide hinge 1 to tackle the complicated PPIs involved in discontinuous epitopes in, for example, antibody–antigen interactions . Through the chemical creation of cyclic peptides corresponding to the amino acid sequence of the epitopes by use of azido di(bromomethyl)benzene ( 4 , N 3 ‐DBMB) and attachment of these to a molecular scaffold, PPI modulators of the HIV‐gp120–CD4 interaction were obtained . Although cyclization of the peptides with the benzylic dibromide hinge 4 was very efficient and clean, solubility problems with the resulting cyclic peptides were encountered, probably caused by the apolar hinge used.…”

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confidence: 99%

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Polar Hinges as Functionalized Conformational Constraints in (Bi)cyclic Peptides

et al. 2017

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Two polar hinges for cyclization of peptides have been developed, leading to bicyclic peptides and cyclized peptides with improved solubility and biological activity. Increasingly, we note that a good aqueous solubility of peptides is an absolute prerequisite, not only to allow handling and purification of our target peptides but also being crucial for biological activity characteristics. Compared to earlier hinges, the 1,1',1"-(1,3,5-triazinane-1,3,5-triyl)tris(2-bromoethanone) (TATB) and 2,4,6-tris(bromomethyl)-s-triazine (TBMT), each containing three nitrogen atoms are structurally similar but chemically very different. Both were accessible in a one-step fashion from bromoacetonitrile. TATB and TBMT are very suitable for the preparation of more soluble bicyclic peptides. Azide-modified TATB and TBMT derivatives provide hinges for the preparation of cyclized peptides for incorporation on scaffolds to afford protein mimics.

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Amide‐Forming Ligation Reactions

2019

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One of the long‐standing pursuits of synthetic organic chemists is the development of chemical methods for the synthesis of peptides and proteins as tools for understanding biological processes and providing therapeutic solutions to human diseases. The advent of chemoselective ligation reactions for the chemical synthesis of peptides and proteins has enabled synthetic chemists to realize this long‐held dream. In an amide‐forming ligation reaction, two uniquely placed functional groups within the peptide allow peptide or protein segments to be joined in a chemoselective manner with an amide bond. In this chapter, some of the early methods based on principles of the capture/rearrangement strategy for ligation of peptides are catalogued, followed by some of the most versatile and well‐established contemporary methods for the preparation of linear/cyclic peptides and proteins such as the native chemical ligation (NCL) and the α‐ketoacid–hydroxylamine (KAHA) ligation. The chapter concludes with some of the most promising new generation ligation methods such as the potassium acyltrifluoroborate–hydroxylamine (KAT) ligation. The tremendous progress in the past two decades in the development of several ligation methods that rely on a pair of unique functional groups is set to expand the horizons of fully functional proteins and multi‐protein assemblies that are purely synthetically prepared. Although contemporary ligation reactions do not match the speed and efficiency at which proteins are assembled in biological systems, the repertoire of chemoselective amide‐forming ligation methods has already enabled synthetic protein chemistry to surpass biology in terms of chemical and structural diversity.

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Molecular construction of HIV-gp120 discontinuous epitope mimics by assembly of cyclic peptides on an orthogonal alkyne functionalized TAC-scaffold

Cited by 16 publications

References 22 publications

Highly potent antimicrobial peptide derivatives of bovine cateslytin

Highly potent antimicrobial peptide derivatives of bovine cateslytin

Polar Hinges as Functionalized Conformational Constraints in (Bi)cyclic Peptides

Amide‐Forming Ligation Reactions

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