A fragment-based selection approach for the discovery of peptide macrocycles targeting protein kinases

Elizabeth Restituyo; Karla Camacho-Soto; Indraneel Ghosh

doi:10.1007/978-1-4939-2020-4_7

A fragment-based selection approach for the discovery of peptide macrocycles targeting protein kinases

Elizabeth Restituyo, Karla Camacho-Soto, Indraneel Ghosh

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

Protein kinases are implicated in diverse signaling cascades and have been targeted with small molecules that typically bind the conserved ATP-binding active site. These inhibitors are often promiscuous and target multiple protein kinases, which has led to the development of alternate strategies to discover selective ligands. We have recently described a fragment-based selection approach, where a small-molecule warhead can be non-covalently tethered to a phage-displayed library of cyclic peptides. This approach led to the conversion of the promiscuous kinase inhibitor, staurosporine, into a selective bivalent inhibitor.

Original language	English (US)
Pages (from-to)	95-104
Number of pages	10
Journal	Methods in Molecular Biology
Volume	1248
DOIs	https://doi.org/10.1007/978-1-4939-2020-4_7
State	Published - 2015

Keywords

Allosteric inhibitors
Bivalent inhibitors
Fragment-based ligand discovery
Peptide macrocycles
Phage display
Protein kinases
Solid-phase peptide synthesis

ASJC Scopus subject areas

Molecular Biology
Genetics

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10.1007/978-1-4939-2020-4_7

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title = "A fragment-based selection approach for the discovery of peptide macrocycles targeting protein kinases",

abstract = "Protein kinases are implicated in diverse signaling cascades and have been targeted with small molecules that typically bind the conserved ATP-binding active site. These inhibitors are often promiscuous and target multiple protein kinases, which has led to the development of alternate strategies to discover selective ligands. We have recently described a fragment-based selection approach, where a small-molecule warhead can be non-covalently tethered to a phage-displayed library of cyclic peptides. This approach led to the conversion of the promiscuous kinase inhibitor, staurosporine, into a selective bivalent inhibitor.",

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AU - Camacho-Soto, Karla

AU - Ghosh, Indraneel

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AB - Protein kinases are implicated in diverse signaling cascades and have been targeted with small molecules that typically bind the conserved ATP-binding active site. These inhibitors are often promiscuous and target multiple protein kinases, which has led to the development of alternate strategies to discover selective ligands. We have recently described a fragment-based selection approach, where a small-molecule warhead can be non-covalently tethered to a phage-displayed library of cyclic peptides. This approach led to the conversion of the promiscuous kinase inhibitor, staurosporine, into a selective bivalent inhibitor.

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A fragment-based selection approach for the discovery of peptide macrocycles targeting protein kinases

Abstract

Keywords

ASJC Scopus subject areas

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