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Macrocyclic peptides that inhibit Wnt signalling via interaction with Wnt3a

Here we report de novo macrocyclic peptide binders to Wnt3a, a member of the Wnt protein family. By means of the Random non-standard Peptides Integrated Discovery (RaPID) system, we have performed in vitro selection against the complex of mouse Wnt3a (mWnt3a) with human afamin (hAFM) to discover mac...

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Autores principales: Otero-Ramirez, Manuel E., Matoba, Kyoko, Mihara, Emiko, Passioura, Toby, Takagi, Junichi, Suga, Hiroaki
Formato: Online Artículo Texto
Lenguaje:English
Publicado: RSC 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8382136/
https://www.ncbi.nlm.nih.gov/pubmed/34458746
http://dx.doi.org/10.1039/d0cb00016g
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author Otero-Ramirez, Manuel E.
Matoba, Kyoko
Mihara, Emiko
Passioura, Toby
Takagi, Junichi
Suga, Hiroaki
author_facet Otero-Ramirez, Manuel E.
Matoba, Kyoko
Mihara, Emiko
Passioura, Toby
Takagi, Junichi
Suga, Hiroaki
author_sort Otero-Ramirez, Manuel E.
collection PubMed
description Here we report de novo macrocyclic peptide binders to Wnt3a, a member of the Wnt protein family. By means of the Random non-standard Peptides Integrated Discovery (RaPID) system, we have performed in vitro selection against the complex of mouse Wnt3a (mWnt3a) with human afamin (hAFM) to discover macrocyclic peptides that bind mWnt3a with K(D) values as tight as 110 nM. One of these peptides, WAp-D04 (Wnt–AFM-peptide-D04), was able to inhibit the receptor-mediated signaling process, which was demonstrated in a Wnt3a-dependent reporter cell-line. Based on this initial hit, we applied a block-mutagenesis scanning display to identify a mutant inhibitor, WAp-D04-W10P, with 5-fold greater potency in a reporter assay. This work represents the first instance of molecules capable of inhibiting Wnt signaling through direct interaction with a Wnt protein, a molecular class for which targeting has been challenging due its highly hydrophobic nature.
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spelling pubmed-83821362021-08-26 Macrocyclic peptides that inhibit Wnt signalling via interaction with Wnt3a Otero-Ramirez, Manuel E. Matoba, Kyoko Mihara, Emiko Passioura, Toby Takagi, Junichi Suga, Hiroaki RSC Chem Biol Chemistry Here we report de novo macrocyclic peptide binders to Wnt3a, a member of the Wnt protein family. By means of the Random non-standard Peptides Integrated Discovery (RaPID) system, we have performed in vitro selection against the complex of mouse Wnt3a (mWnt3a) with human afamin (hAFM) to discover macrocyclic peptides that bind mWnt3a with K(D) values as tight as 110 nM. One of these peptides, WAp-D04 (Wnt–AFM-peptide-D04), was able to inhibit the receptor-mediated signaling process, which was demonstrated in a Wnt3a-dependent reporter cell-line. Based on this initial hit, we applied a block-mutagenesis scanning display to identify a mutant inhibitor, WAp-D04-W10P, with 5-fold greater potency in a reporter assay. This work represents the first instance of molecules capable of inhibiting Wnt signaling through direct interaction with a Wnt protein, a molecular class for which targeting has been challenging due its highly hydrophobic nature. RSC 2020-03-24 /pmc/articles/PMC8382136/ /pubmed/34458746 http://dx.doi.org/10.1039/d0cb00016g Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Otero-Ramirez, Manuel E.
Matoba, Kyoko
Mihara, Emiko
Passioura, Toby
Takagi, Junichi
Suga, Hiroaki
Macrocyclic peptides that inhibit Wnt signalling via interaction with Wnt3a
title Macrocyclic peptides that inhibit Wnt signalling via interaction with Wnt3a
title_full Macrocyclic peptides that inhibit Wnt signalling via interaction with Wnt3a
title_fullStr Macrocyclic peptides that inhibit Wnt signalling via interaction with Wnt3a
title_full_unstemmed Macrocyclic peptides that inhibit Wnt signalling via interaction with Wnt3a
title_short Macrocyclic peptides that inhibit Wnt signalling via interaction with Wnt3a
title_sort macrocyclic peptides that inhibit wnt signalling via interaction with wnt3a
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8382136/
https://www.ncbi.nlm.nih.gov/pubmed/34458746
http://dx.doi.org/10.1039/d0cb00016g
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