Peptide Ligands Stabilized by Small Molecules

Chen, Shiyu; Bertoldo, Davide; Angelini, Alessandro; Pojer, F.; Heinis, Christian

doi:10.1002/ange.201309459

Cited by 49 publications

(36 citation statements)

References 18 publications

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“…The use of 1,3,5-trisbromomethylbenzene (TBMB) 37 to generate bicyclic phage displayed libraries has been used to develop high affinity ligands specific for human plasma kallikrein 38 and human urokinase-type plasminogen activator 18, 39 . Similar strategies involving 1,3,5-triacryloyl-1,3,5-triazinane (TATA) and N , N ′, N ″-(benzene-1,3,5-triyl)-tris(2-bromoacetamide) (TBAB) have also been reported 40 . While the size of each macrocycle can be varied using these linkers, conformations are limited to two independent loops because of the reliance on a central, trisubstituted linker.…”

Section: Introductionmentioning

confidence: 71%

Highly Constrained Bicyclic Scaffolds for the Discovery of Protease-Stable Peptides via mRNA Display

et al. 2017

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Highly-constrained peptides such as the knotted peptide natural products are promising medicinal agents because of their impressive biostability and potent activity. Yet, libraries of highly-constrained peptides are challenging to prepare. Here we present a method which utilizes two robust, orthogonal chemical steps to create highly-constrained bicyclic peptide libraries. This technology was optimized to be compatible with in vitro selections by mRNA display. We performed side-by-side monocyclic and bicyclic selections against a model protein (streptavidin). Both selections resulted in peptides with mid nM affinity, and the bicyclic selection yielded a peptide with remarkable protease resistance.

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Section: Introductionmentioning

confidence: 71%

Highly Constrained Bicyclic Scaffolds for the Discovery of Protease-Stable Peptides via mRNA Display

et al. 2017

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“…The inhibitors of PK and uPA even did not inhibit the murine orthologs [14,38 ]. X-ray structures of bicyclic peptides with their targets showed a high shape complementarity of peptide and target, and explained the good target selectivity (Figure 4b) [14,42].…”

Section: Bicyclic Peptidesmentioning

confidence: 92%

“…Like TBMB, TATA and TBAB were shown to efficiently and selectively cyclize peptides containing three cysteines [46]. Panning of peptide phage libraries cyclized with either TBMB, TATA or TBAB against the target uPA yielded entirely different families of ligands [42]. Most of the isolated peptides bound the target only when cyclized with the linker that was used in the selection but not when cyclized with one of the other two linkers.…”

Section: Bicyclic Peptidesmentioning

confidence: 98%

“…Most of the isolated peptides bound the target only when cyclized with the linker that was used in the selection but not when cyclized with one of the other two linkers. X-ray crystallographic analysis of the bicyclic peptides in complex with uPA showed that some of the linkers played important structural roles; in one peptide, the linker even formed Hbonds with the peptide and the target protein [42].…”

Section: Bicyclic Peptidesmentioning

confidence: 99%

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Encoded libraries of chemically modified peptides

Heinis

Winter

2015

Current Opinion in Chemical Biology

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116

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“…We describe here a general, unbiased approach to directly screen pools of covalent probes with exceptional diversity using the power of phage display. Inspired by the work of others in which phage are chemically modified to produce cyclic and bicyclic peptides directly on the phage surface [21][22][23][24], we developed a small molecule linker that could be used to both form cyclic peptides and also introduce a weak electrophile 'warhead' directly on the cyclized phage coat protein segment ( Fig. 1).…”

Section: Introductionmentioning

confidence: 99%

A phage display approach to identify highly selective covalent binders

Chen

Bogyo

2019

Preprint

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Molecules that bind macromolecular targets through direct covalent modification have found widespread applications as activity-based probes (ABPs) and as irreversible drugs. Covalent binders can be used to dynamically monitor the activity of enzymes in complex cellular environments, identify targets and induce permanent binding/inhibition of therapeutically important biomolecules. However, the general reactivity of the electrophiles needed for covalent bond formation makes control of selectivity difficult. There is currently no rapid, robust and unbiased screening method to identify new classes of covalent binding ligands from highly diverse pools of candidate molecules. Here we describe the development of a phage display method to screen for highly selective covalent binding ligands. This approach makes use of a reactive linker to form cyclic peptides on the phage surface while simultaneously introducing an electrophilic 'warhead' to covalently react with a nucleophile on the target. Using this approach, we identified cyclic peptides that selectively and irreversibly inhibited a cysteine protease with nanomolar potency, exceptional specificity and increased serum stability compared to a linear peptide containing the same electrophile. This approach should enable rapid, unbiased screening to identify new classes of highly selective covalent binding ligands for diverse molecular targets.

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Peptide Ligands Stabilized by Small Molecules

Cited by 49 publications

References 18 publications

Highly Constrained Bicyclic Scaffolds for the Discovery of Protease-Stable Peptides via mRNA Display

Highly Constrained Bicyclic Scaffolds for the Discovery of Protease-Stable Peptides via mRNA Display

Encoded libraries of chemically modified peptides

A phage display approach to identify highly selective covalent binders

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