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Low-dose in situ prelocation of protein microcrystals by 2D X-ray phase-contrast imaging for serial crystallography

Serial protein crystallography has emerged as a powerful method of data collection on small crystals from challenging targets, such as membrane proteins. Multiple microcrystals need to be located on large and often flat mounts while exposing them to an X-ray dose that is as low as possible. A crysta...

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Autores principales: Martiel, Isabelle, Huang, Chia-Ying, Villanueva-Perez, Pablo, Panepucci, Ezequiel, Basu, Shibom, Caffrey, Martin, Pedrini, Bill, Bunk, Oliver, Stampanoni, Marco, Wang, Meitian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: International Union of Crystallography 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7642777/
https://www.ncbi.nlm.nih.gov/pubmed/33209324
http://dx.doi.org/10.1107/S2052252520013238
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author Martiel, Isabelle
Huang, Chia-Ying
Villanueva-Perez, Pablo
Panepucci, Ezequiel
Basu, Shibom
Caffrey, Martin
Pedrini, Bill
Bunk, Oliver
Stampanoni, Marco
Wang, Meitian
author_facet Martiel, Isabelle
Huang, Chia-Ying
Villanueva-Perez, Pablo
Panepucci, Ezequiel
Basu, Shibom
Caffrey, Martin
Pedrini, Bill
Bunk, Oliver
Stampanoni, Marco
Wang, Meitian
author_sort Martiel, Isabelle
collection PubMed
description Serial protein crystallography has emerged as a powerful method of data collection on small crystals from challenging targets, such as membrane proteins. Multiple microcrystals need to be located on large and often flat mounts while exposing them to an X-ray dose that is as low as possible. A crystal-prelocation method is demonstrated here using low-dose 2D full-field propagation-based X-ray phase-contrast imaging at the X-ray imaging beamline TOMCAT at the Swiss Light Source (SLS). This imaging step provides microcrystal coordinates for automated serial data collection at a microfocus macromolecular crystallography beamline on samples with an essentially flat geometry. This prelocation method was applied to microcrystals of a soluble protein and a membrane protein, grown in a commonly used double-sandwich in situ crystallization plate. The inner sandwiches of thin plastic film enclosing the microcrystals in lipid cubic phase were flash cooled and imaged at TOMCAT. Based on the obtained crystal coordinates, both still and rotation wedge serial data were collected automatically at the SLS PXI beamline, yielding in both cases a high indexing rate. This workflow can be easily implemented at many synchrotron facilities using existing equipment, or potentially integrated as an online technique in the next-generation macromolecular crystallography beamline, and thus benefit a number of dose-sensitive challenging protein targets.
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spelling pubmed-76427772020-11-17 Low-dose in situ prelocation of protein microcrystals by 2D X-ray phase-contrast imaging for serial crystallography Martiel, Isabelle Huang, Chia-Ying Villanueva-Perez, Pablo Panepucci, Ezequiel Basu, Shibom Caffrey, Martin Pedrini, Bill Bunk, Oliver Stampanoni, Marco Wang, Meitian IUCrJ Research Papers Serial protein crystallography has emerged as a powerful method of data collection on small crystals from challenging targets, such as membrane proteins. Multiple microcrystals need to be located on large and often flat mounts while exposing them to an X-ray dose that is as low as possible. A crystal-prelocation method is demonstrated here using low-dose 2D full-field propagation-based X-ray phase-contrast imaging at the X-ray imaging beamline TOMCAT at the Swiss Light Source (SLS). This imaging step provides microcrystal coordinates for automated serial data collection at a microfocus macromolecular crystallography beamline on samples with an essentially flat geometry. This prelocation method was applied to microcrystals of a soluble protein and a membrane protein, grown in a commonly used double-sandwich in situ crystallization plate. The inner sandwiches of thin plastic film enclosing the microcrystals in lipid cubic phase were flash cooled and imaged at TOMCAT. Based on the obtained crystal coordinates, both still and rotation wedge serial data were collected automatically at the SLS PXI beamline, yielding in both cases a high indexing rate. This workflow can be easily implemented at many synchrotron facilities using existing equipment, or potentially integrated as an online technique in the next-generation macromolecular crystallography beamline, and thus benefit a number of dose-sensitive challenging protein targets. International Union of Crystallography 2020-10-23 /pmc/articles/PMC7642777/ /pubmed/33209324 http://dx.doi.org/10.1107/S2052252520013238 Text en © Martiel et al. 2020 http://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.http://creativecommons.org/licenses/by/4.0/
spellingShingle Research Papers
Martiel, Isabelle
Huang, Chia-Ying
Villanueva-Perez, Pablo
Panepucci, Ezequiel
Basu, Shibom
Caffrey, Martin
Pedrini, Bill
Bunk, Oliver
Stampanoni, Marco
Wang, Meitian
Low-dose in situ prelocation of protein microcrystals by 2D X-ray phase-contrast imaging for serial crystallography
title Low-dose in situ prelocation of protein microcrystals by 2D X-ray phase-contrast imaging for serial crystallography
title_full Low-dose in situ prelocation of protein microcrystals by 2D X-ray phase-contrast imaging for serial crystallography
title_fullStr Low-dose in situ prelocation of protein microcrystals by 2D X-ray phase-contrast imaging for serial crystallography
title_full_unstemmed Low-dose in situ prelocation of protein microcrystals by 2D X-ray phase-contrast imaging for serial crystallography
title_short Low-dose in situ prelocation of protein microcrystals by 2D X-ray phase-contrast imaging for serial crystallography
title_sort low-dose in situ prelocation of protein microcrystals by 2d x-ray phase-contrast imaging for serial crystallography
topic Research Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7642777/
https://www.ncbi.nlm.nih.gov/pubmed/33209324
http://dx.doi.org/10.1107/S2052252520013238
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