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Getting a Grip on the Undrugged: Targeting β‐Catenin with Fragment‐Based Methods

Aberrant WNT pathway activation, leading to nuclear accumulation of β‐catenin, is a key oncogenic driver event. Mutations in the tumor suppressor gene APC lead to impaired proteasomal degradation of β‐catenin and subsequent nuclear translocation. Restoring cellular degradation of β‐catenin represent...

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Autores principales: Kessler, Dirk, Mayer, Moriz, Zahn, Stephan K., Zeeb, Markus, Wöhrle, Simon, Bergner, Andreas, Bruchhaus, Jens, Ciftci, Tuncay, Dahmann, Georg, Dettling, Maike, Döbel, Sandra, Fuchs, Julian E., Geist, Leonhard, Hela, Wolfgang, Kofink, Christiane, Kousek, Roland, Moser, Franziska, Puchner, Teresa, Rumpel, Klaus, Scharnweber, Maximilian, Werni, Patrick, Wolkerstorfer, Bernhard, Breitsprecher, Dennis, Baaske, Philipp, Pearson, Mark, McConnell, Darryl B., Böttcher, Jark
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8247886/
https://www.ncbi.nlm.nih.gov/pubmed/33275320
http://dx.doi.org/10.1002/cmdc.202000839
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author Kessler, Dirk
Mayer, Moriz
Zahn, Stephan K.
Zeeb, Markus
Wöhrle, Simon
Bergner, Andreas
Bruchhaus, Jens
Ciftci, Tuncay
Dahmann, Georg
Dettling, Maike
Döbel, Sandra
Fuchs, Julian E.
Geist, Leonhard
Hela, Wolfgang
Kofink, Christiane
Kousek, Roland
Moser, Franziska
Puchner, Teresa
Rumpel, Klaus
Scharnweber, Maximilian
Werni, Patrick
Wolkerstorfer, Bernhard
Breitsprecher, Dennis
Baaske, Philipp
Pearson, Mark
McConnell, Darryl B.
Böttcher, Jark
author_facet Kessler, Dirk
Mayer, Moriz
Zahn, Stephan K.
Zeeb, Markus
Wöhrle, Simon
Bergner, Andreas
Bruchhaus, Jens
Ciftci, Tuncay
Dahmann, Georg
Dettling, Maike
Döbel, Sandra
Fuchs, Julian E.
Geist, Leonhard
Hela, Wolfgang
Kofink, Christiane
Kousek, Roland
Moser, Franziska
Puchner, Teresa
Rumpel, Klaus
Scharnweber, Maximilian
Werni, Patrick
Wolkerstorfer, Bernhard
Breitsprecher, Dennis
Baaske, Philipp
Pearson, Mark
McConnell, Darryl B.
Böttcher, Jark
author_sort Kessler, Dirk
collection PubMed
description Aberrant WNT pathway activation, leading to nuclear accumulation of β‐catenin, is a key oncogenic driver event. Mutations in the tumor suppressor gene APC lead to impaired proteasomal degradation of β‐catenin and subsequent nuclear translocation. Restoring cellular degradation of β‐catenin represents a potential therapeutic strategy. Here, we report the fragment‐based discovery of a small molecule binder to β‐catenin, including the structural elucidation of the binding mode by X‐ray crystallography. The difficulty in drugging β‐catenin was confirmed as the primary screening campaigns identified only few and very weak hits. Iterative virtual and NMR screening techniques were required to discover a compound with sufficient potency to be able to obtain an X‐ray co‐crystal structure. The binding site is located between armadillo repeats two and three, adjacent to the BCL9 and TCF4 binding sites. Genetic studies show that it is unlikely to be useful for the development of protein–protein interaction inhibitors but structural information and established assays provide a solid basis for a prospective optimization towards β‐catenin proteolysis targeting chimeras (PROTACs) as alternative modality.
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spelling pubmed-82478862021-07-02 Getting a Grip on the Undrugged: Targeting β‐Catenin with Fragment‐Based Methods Kessler, Dirk Mayer, Moriz Zahn, Stephan K. Zeeb, Markus Wöhrle, Simon Bergner, Andreas Bruchhaus, Jens Ciftci, Tuncay Dahmann, Georg Dettling, Maike Döbel, Sandra Fuchs, Julian E. Geist, Leonhard Hela, Wolfgang Kofink, Christiane Kousek, Roland Moser, Franziska Puchner, Teresa Rumpel, Klaus Scharnweber, Maximilian Werni, Patrick Wolkerstorfer, Bernhard Breitsprecher, Dennis Baaske, Philipp Pearson, Mark McConnell, Darryl B. Böttcher, Jark ChemMedChem Communications Aberrant WNT pathway activation, leading to nuclear accumulation of β‐catenin, is a key oncogenic driver event. Mutations in the tumor suppressor gene APC lead to impaired proteasomal degradation of β‐catenin and subsequent nuclear translocation. Restoring cellular degradation of β‐catenin represents a potential therapeutic strategy. Here, we report the fragment‐based discovery of a small molecule binder to β‐catenin, including the structural elucidation of the binding mode by X‐ray crystallography. The difficulty in drugging β‐catenin was confirmed as the primary screening campaigns identified only few and very weak hits. Iterative virtual and NMR screening techniques were required to discover a compound with sufficient potency to be able to obtain an X‐ray co‐crystal structure. The binding site is located between armadillo repeats two and three, adjacent to the BCL9 and TCF4 binding sites. Genetic studies show that it is unlikely to be useful for the development of protein–protein interaction inhibitors but structural information and established assays provide a solid basis for a prospective optimization towards β‐catenin proteolysis targeting chimeras (PROTACs) as alternative modality. John Wiley and Sons Inc. 2021-01-14 2021-05-06 /pmc/articles/PMC8247886/ /pubmed/33275320 http://dx.doi.org/10.1002/cmdc.202000839 Text en © 2020 The Authors. ChemMedChem published by Wiley-VCH GmbH https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Communications
Kessler, Dirk
Mayer, Moriz
Zahn, Stephan K.
Zeeb, Markus
Wöhrle, Simon
Bergner, Andreas
Bruchhaus, Jens
Ciftci, Tuncay
Dahmann, Georg
Dettling, Maike
Döbel, Sandra
Fuchs, Julian E.
Geist, Leonhard
Hela, Wolfgang
Kofink, Christiane
Kousek, Roland
Moser, Franziska
Puchner, Teresa
Rumpel, Klaus
Scharnweber, Maximilian
Werni, Patrick
Wolkerstorfer, Bernhard
Breitsprecher, Dennis
Baaske, Philipp
Pearson, Mark
McConnell, Darryl B.
Böttcher, Jark
Getting a Grip on the Undrugged: Targeting β‐Catenin with Fragment‐Based Methods
title Getting a Grip on the Undrugged: Targeting β‐Catenin with Fragment‐Based Methods
title_full Getting a Grip on the Undrugged: Targeting β‐Catenin with Fragment‐Based Methods
title_fullStr Getting a Grip on the Undrugged: Targeting β‐Catenin with Fragment‐Based Methods
title_full_unstemmed Getting a Grip on the Undrugged: Targeting β‐Catenin with Fragment‐Based Methods
title_short Getting a Grip on the Undrugged: Targeting β‐Catenin with Fragment‐Based Methods
title_sort getting a grip on the undrugged: targeting β‐catenin with fragment‐based methods
topic Communications
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8247886/
https://www.ncbi.nlm.nih.gov/pubmed/33275320
http://dx.doi.org/10.1002/cmdc.202000839
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