Probing ligand binding of endothiapepsin by ‘temperature-resolved’ macromolecular crystallography

Continuous developments in cryogenic X-ray crystallography have provided most of our knowledge of 3D protein structures, which has recently been further augmented by revolutionary advances in cryoEM. However, a single structural conformation identified at cryogenic temperatures may introduce a ficti...

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Autores principales: Huang, Chia-Ying, Aumonier, Sylvain, Engilberge, Sylvain, Eris, Deniz, Smith, Kate Mary Louise, Leonarski, Filip, Wojdyla, Justyna Aleksandra, Beale, John H., Buntschu, Dominik, Pauluhn, Anuschka, Sharpe, May Elizabeth, Metz, Alexander, Olieric, Vincent, Wang, Meitian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: International Union of Crystallography 2022
Materias:
Research Papers
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9344481/
https://www.ncbi.nlm.nih.gov/pubmed/35916221
http://dx.doi.org/10.1107/S205979832200612X
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author Huang, Chia-Ying
Aumonier, Sylvain
Engilberge, Sylvain
Eris, Deniz
Smith, Kate Mary Louise
Leonarski, Filip
Wojdyla, Justyna Aleksandra
Beale, John H.
Buntschu, Dominik
Pauluhn, Anuschka
Sharpe, May Elizabeth
Metz, Alexander
Olieric, Vincent
Wang, Meitian
author_facet Huang, Chia-Ying
Aumonier, Sylvain
Engilberge, Sylvain
Eris, Deniz
Smith, Kate Mary Louise
Leonarski, Filip
Wojdyla, Justyna Aleksandra
Beale, John H.
Buntschu, Dominik
Pauluhn, Anuschka
Sharpe, May Elizabeth
Metz, Alexander
Olieric, Vincent
Wang, Meitian
author_sort Huang, Chia-Ying
collection PubMed
description Continuous developments in cryogenic X-ray crystallography have provided most of our knowledge of 3D protein structures, which has recently been further augmented by revolutionary advances in cryoEM. However, a single structural conformation identified at cryogenic temperatures may introduce a fictitious structure as a result of cryogenic cooling artefacts, limiting the overview of inherent protein physiological dynamics, which play a critical role in the biological functions of proteins. Here, a room-temperature X-ray crystallo­graphic method using temperature as a trigger to record movie-like structural snapshots has been developed. The method has been used to show how TL00150, a 175.15 Da fragment, undergoes binding-mode changes in endothiapepsin. A surprising fragment-binding discrepancy was observed between the cryo-cooled and physiological temperature structures, and multiple binding poses and their interplay with DMSO were captured. The observations here open up new promising prospects for structure determination and interpretation at physiological temperatures with implications for structure-based drug discovery.
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spelling pubmed-93444812022-08-15 Probing ligand binding of endothiapepsin by ‘temperature-resolved’ macromolecular crystallography Huang, Chia-Ying Aumonier, Sylvain Engilberge, Sylvain Eris, Deniz Smith, Kate Mary Louise Leonarski, Filip Wojdyla, Justyna Aleksandra Beale, John H. Buntschu, Dominik Pauluhn, Anuschka Sharpe, May Elizabeth Metz, Alexander Olieric, Vincent Wang, Meitian Acta Crystallogr D Struct Biol Research Papers Continuous developments in cryogenic X-ray crystallography have provided most of our knowledge of 3D protein structures, which has recently been further augmented by revolutionary advances in cryoEM. However, a single structural conformation identified at cryogenic temperatures may introduce a fictitious structure as a result of cryogenic cooling artefacts, limiting the overview of inherent protein physiological dynamics, which play a critical role in the biological functions of proteins. Here, a room-temperature X-ray crystallo­graphic method using temperature as a trigger to record movie-like structural snapshots has been developed. The method has been used to show how TL00150, a 175.15 Da fragment, undergoes binding-mode changes in endothiapepsin. A surprising fragment-binding discrepancy was observed between the cryo-cooled and physiological temperature structures, and multiple binding poses and their interplay with DMSO were captured. The observations here open up new promising prospects for structure determination and interpretation at physiological temperatures with implications for structure-based drug discovery. International Union of Crystallography 2022-07-27 /pmc/articles/PMC9344481/ /pubmed/35916221 http://dx.doi.org/10.1107/S205979832200612X Text en © Chia-Ying Huang et al. 2022 https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution (CC-BY) Licence, which permits unrestricted use, distribution, and reproduction in any medium, provided the original authors and source are cited.
spellingShingle Research Papers
Huang, Chia-Ying
Aumonier, Sylvain
Engilberge, Sylvain
Eris, Deniz
Smith, Kate Mary Louise
Leonarski, Filip
Wojdyla, Justyna Aleksandra
Beale, John H.
Buntschu, Dominik
Pauluhn, Anuschka
Sharpe, May Elizabeth
Metz, Alexander
Olieric, Vincent
Wang, Meitian
Probing ligand binding of endothiapepsin by ‘temperature-resolved’ macromolecular crystallography
title Probing ligand binding of endothiapepsin by ‘temperature-resolved’ macromolecular crystallography
title_full Probing ligand binding of endothiapepsin by ‘temperature-resolved’ macromolecular crystallography
title_fullStr Probing ligand binding of endothiapepsin by ‘temperature-resolved’ macromolecular crystallography
title_full_unstemmed Probing ligand binding of endothiapepsin by ‘temperature-resolved’ macromolecular crystallography
title_short Probing ligand binding of endothiapepsin by ‘temperature-resolved’ macromolecular crystallography
title_sort probing ligand binding of endothiapepsin by ‘temperature-resolved’ macromolecular crystallography
topic Research Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9344481/
https://www.ncbi.nlm.nih.gov/pubmed/35916221
http://dx.doi.org/10.1107/S205979832200612X
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