Serial millisecond crystallography of membrane and soluble protein microcrystals using synchrotron radiation

Jose M. Martin-Garcia; Chelsie E. Conrad; Garrett Nelson; Natasha Stander; Nadia Zatsepin; James Zook; Lan Zhu; James Geiger; Eugene Chun; David Kissick; Mark C. Hilgart; Craig Ogata; Andrii Ishchenko; Nirupa Nagaratnam; Shatabdi Roy-Chowdhury; Jesse Coe; Ganesh Subramanian; Alexander Schaffer; Daniel James; Gihan Ketwala; Nagarajan Venugopalan; Shenglan Xu; Stephen Corcoran; Dale Ferguson; Uwe Weierstall; John Spence; Vadim Cherezov; Petra Fromme; Robert F. Fischetti; Wei Liu

doi:10.1107/S205225251700570X

Serial millisecond crystallography of membrane and soluble protein microcrystals using synchrotron radiation

Jose M. Martin-Garcia, Chelsie E. Conrad, Garrett Nelson, Natasha Stander, Nadia Zatsepin, James Zook, Lan Zhu, James Geiger, Eugene Chun, David Kissick, Mark C. Hilgart, Craig Ogata, Andrii Ishchenko, Nirupa Nagaratnam, Shatabdi Roy-Chowdhury, Jesse Coe, Ganesh Subramanian, Alexander Schaffer, Daniel James, Gihan KetwalaNagarajan Venugopalan, Shenglan Xu, Stephen Corcoran, Dale Ferguson, Uwe Weierstall, John Spence, Vadim Cherezov, Petra Fromme, Robert F. Fischetti, Wei Liu

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

112 Scopus citations

Abstract

Crystal structure determination of biological macromolecules using the novel technique of serial femtosecond crystallography (SFX) is severely limited by the scarcity of X-ray free-electron laser (XFEL) sources. However, recent and future upgrades render microfocus beamlines at synchrotron-radiation sources suitable for room-temperature serial crystallography data collection also. Owing to the longer exposure times that are needed at synchrotrons, serial data collection is termed serial millisecond crystallography (SMX). As a result, the number of SMX experiments is growing rapidly, with a dozen experiments reported so far. Here, the first high-viscosity injector-based SMX experiments carried out at a US synchrotron source, the Advanced Photon Source (APS), are reported. Microcrystals (5-20μm) of a wide variety of proteins, including lysozyme, thaumatin, phycocyanin, the human A 2A adenosine receptor (A 2A AR), the soluble fragment of the membrane lipoprotein Flpp3 and proteinase K, were screened. Crystals suspended in lipidic cubic phase (LCP) or a high-molecular-weight poly(ethylene oxide) (PEO; molecular weight 8000000) were delivered to the beam using a high-viscosity injector. In-house data-reduction (hit-finding) software developed at APS as well as the SFX data-reduction and analysis software suites Cheetah and CrystFEL enabled efficient on-site SMX data monitoring, reduction and processing. Complete data sets were collected for A 2A AR, phycocyanin, Flpp3, proteinase K and lysozyme, and the structures of A 2A AR, phycocyanin, proteinase K and lysozyme were determined at 3.2, 3.1, 2.65 and 2.05Å resolution, respectively. The data demonstrate the feasibility of serial millisecond crystallography from 5-20μm crystals using a high-viscosity injector at APS. The resolution of the crystal structures obtained in this study was dictated by the current flux density and crystal size, but upcoming developments in beamline optics and the planned APS-U upgrade will increase the intensity by two orders of magnitude. These developments will enable structure determination from smaller and/or weakly diffracting microcrystals.

Original language	English (US)
Pages (from-to)	439-454
Number of pages	16
Journal	IUCrJ
Volume	4
DOIs	https://doi.org/10.1107/S205225251700570X
State	Published - 2017

Keywords

Advanced Photon Source
high-viscosity injector
serial millisecond crystallography
synchrotron radiation

ASJC Scopus subject areas

General Chemistry
Biochemistry
General Materials Science
Condensed Matter Physics

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10.1107/S205225251700570X

Cite this

Martin-Garcia, J. M., Conrad, C. E., Nelson, G., Stander, N., Zatsepin, N., Zook, J., Zhu, L., Geiger, J., Chun, E., Kissick, D., Hilgart, M. C., Ogata, C., Ishchenko, A., Nagaratnam, N., Roy-Chowdhury, S., Coe, J., Subramanian, G., Schaffer, A., James, D., ... Liu, W. (2017). Serial millisecond crystallography of membrane and soluble protein microcrystals using synchrotron radiation. IUCrJ, 4, 439-454. https://doi.org/10.1107/S205225251700570X

Martin-Garcia, JM, Conrad, CE, Nelson, G, Stander, N, Zatsepin, N, Zook, J, Zhu, L, Geiger, J, Chun, E, Kissick, D, Hilgart, MC, Ogata, C, Ishchenko, A, Nagaratnam, N, Roy-Chowdhury, S, Coe, J, Subramanian, G, Schaffer, A, James, D, Ketwala, G, Venugopalan, N, Xu, S, Corcoran, S, Ferguson, D, Weierstall, U, Spence, J, Cherezov, V, Fromme, P, Fischetti, RF & Liu, W 2017, 'Serial millisecond crystallography of membrane and soluble protein microcrystals using synchrotron radiation', IUCrJ, vol. 4, pp. 439-454. https://doi.org/10.1107/S205225251700570X

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title = "Serial millisecond crystallography of membrane and soluble protein microcrystals using synchrotron radiation",

abstract = "Crystal structure determination of biological macromolecules using the novel technique of serial femtosecond crystallography (SFX) is severely limited by the scarcity of X-ray free-electron laser (XFEL) sources. However, recent and future upgrades render microfocus beamlines at synchrotron-radiation sources suitable for room-temperature serial crystallography data collection also. Owing to the longer exposure times that are needed at synchrotrons, serial data collection is termed serial millisecond crystallography (SMX). As a result, the number of SMX experiments is growing rapidly, with a dozen experiments reported so far. Here, the first high-viscosity injector-based SMX experiments carried out at a US synchrotron source, the Advanced Photon Source (APS), are reported. Microcrystals (5-20μm) of a wide variety of proteins, including lysozyme, thaumatin, phycocyanin, the human A 2A adenosine receptor (A 2A AR), the soluble fragment of the membrane lipoprotein Flpp3 and proteinase K, were screened. Crystals suspended in lipidic cubic phase (LCP) or a high-molecular-weight poly(ethylene oxide) (PEO; molecular weight 8000000) were delivered to the beam using a high-viscosity injector. In-house data-reduction (hit-finding) software developed at APS as well as the SFX data-reduction and analysis software suites Cheetah and CrystFEL enabled efficient on-site SMX data monitoring, reduction and processing. Complete data sets were collected for A 2A AR, phycocyanin, Flpp3, proteinase K and lysozyme, and the structures of A 2A AR, phycocyanin, proteinase K and lysozyme were determined at 3.2, 3.1, 2.65 and 2.05{\AA} resolution, respectively. The data demonstrate the feasibility of serial millisecond crystallography from 5-20μm crystals using a high-viscosity injector at APS. The resolution of the crystal structures obtained in this study was dictated by the current flux density and crystal size, but upcoming developments in beamline optics and the planned APS-U upgrade will increase the intensity by two orders of magnitude. These developments will enable structure determination from smaller and/or weakly diffracting microcrystals.",

keywords = "Advanced Photon Source, high-viscosity injector, serial millisecond crystallography, synchrotron radiation",

author = "Martin-Garcia, {Jose M.} and Conrad, {Chelsie E.} and Garrett Nelson and Natasha Stander and Nadia Zatsepin and James Zook and Lan Zhu and James Geiger and Eugene Chun and David Kissick and Hilgart, {Mark C.} and Craig Ogata and Andrii Ishchenko and Nirupa Nagaratnam and Shatabdi Roy-Chowdhury and Jesse Coe and Ganesh Subramanian and Alexander Schaffer and Daniel James and Gihan Ketwala and Nagarajan Venugopalan and Shenglan Xu and Stephen Corcoran and Dale Ferguson and Uwe Weierstall and John Spence and Vadim Cherezov and Petra Fromme and Fischetti, {Robert F.} and Wei Liu",

note = "Publisher Copyright: {\textcopyright} Jose M. Martin-Garcia et al. 2017.",

year = "2017",

doi = "10.1107/S205225251700570X",

language = "English (US)",

volume = "4",

pages = "439--454",

journal = "IUCrJ",

issn = "2052-2525",

publisher = "International Union of Crystallography",

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TY - JOUR

T1 - Serial millisecond crystallography of membrane and soluble protein microcrystals using synchrotron radiation

AU - Martin-Garcia, Jose M.

AU - Conrad, Chelsie E.

AU - Nelson, Garrett

AU - Stander, Natasha

AU - Zatsepin, Nadia

AU - Zook, James

AU - Zhu, Lan

AU - Geiger, James

AU - Chun, Eugene

AU - Kissick, David

AU - Hilgart, Mark C.

AU - Ogata, Craig

AU - Ishchenko, Andrii

AU - Nagaratnam, Nirupa

AU - Roy-Chowdhury, Shatabdi

AU - Coe, Jesse

AU - Subramanian, Ganesh

AU - Schaffer, Alexander

AU - James, Daniel

AU - Ketwala, Gihan

AU - Venugopalan, Nagarajan

AU - Xu, Shenglan

AU - Corcoran, Stephen

AU - Ferguson, Dale

AU - Weierstall, Uwe

AU - Spence, John

AU - Cherezov, Vadim

AU - Fromme, Petra

AU - Fischetti, Robert F.

AU - Liu, Wei

PY - 2017

Y1 - 2017

N2 - Crystal structure determination of biological macromolecules using the novel technique of serial femtosecond crystallography (SFX) is severely limited by the scarcity of X-ray free-electron laser (XFEL) sources. However, recent and future upgrades render microfocus beamlines at synchrotron-radiation sources suitable for room-temperature serial crystallography data collection also. Owing to the longer exposure times that are needed at synchrotrons, serial data collection is termed serial millisecond crystallography (SMX). As a result, the number of SMX experiments is growing rapidly, with a dozen experiments reported so far. Here, the first high-viscosity injector-based SMX experiments carried out at a US synchrotron source, the Advanced Photon Source (APS), are reported. Microcrystals (5-20μm) of a wide variety of proteins, including lysozyme, thaumatin, phycocyanin, the human A 2A adenosine receptor (A 2A AR), the soluble fragment of the membrane lipoprotein Flpp3 and proteinase K, were screened. Crystals suspended in lipidic cubic phase (LCP) or a high-molecular-weight poly(ethylene oxide) (PEO; molecular weight 8000000) were delivered to the beam using a high-viscosity injector. In-house data-reduction (hit-finding) software developed at APS as well as the SFX data-reduction and analysis software suites Cheetah and CrystFEL enabled efficient on-site SMX data monitoring, reduction and processing. Complete data sets were collected for A 2A AR, phycocyanin, Flpp3, proteinase K and lysozyme, and the structures of A 2A AR, phycocyanin, proteinase K and lysozyme were determined at 3.2, 3.1, 2.65 and 2.05Å resolution, respectively. The data demonstrate the feasibility of serial millisecond crystallography from 5-20μm crystals using a high-viscosity injector at APS. The resolution of the crystal structures obtained in this study was dictated by the current flux density and crystal size, but upcoming developments in beamline optics and the planned APS-U upgrade will increase the intensity by two orders of magnitude. These developments will enable structure determination from smaller and/or weakly diffracting microcrystals.

AB - Crystal structure determination of biological macromolecules using the novel technique of serial femtosecond crystallography (SFX) is severely limited by the scarcity of X-ray free-electron laser (XFEL) sources. However, recent and future upgrades render microfocus beamlines at synchrotron-radiation sources suitable for room-temperature serial crystallography data collection also. Owing to the longer exposure times that are needed at synchrotrons, serial data collection is termed serial millisecond crystallography (SMX). As a result, the number of SMX experiments is growing rapidly, with a dozen experiments reported so far. Here, the first high-viscosity injector-based SMX experiments carried out at a US synchrotron source, the Advanced Photon Source (APS), are reported. Microcrystals (5-20μm) of a wide variety of proteins, including lysozyme, thaumatin, phycocyanin, the human A 2A adenosine receptor (A 2A AR), the soluble fragment of the membrane lipoprotein Flpp3 and proteinase K, were screened. Crystals suspended in lipidic cubic phase (LCP) or a high-molecular-weight poly(ethylene oxide) (PEO; molecular weight 8000000) were delivered to the beam using a high-viscosity injector. In-house data-reduction (hit-finding) software developed at APS as well as the SFX data-reduction and analysis software suites Cheetah and CrystFEL enabled efficient on-site SMX data monitoring, reduction and processing. Complete data sets were collected for A 2A AR, phycocyanin, Flpp3, proteinase K and lysozyme, and the structures of A 2A AR, phycocyanin, proteinase K and lysozyme were determined at 3.2, 3.1, 2.65 and 2.05Å resolution, respectively. The data demonstrate the feasibility of serial millisecond crystallography from 5-20μm crystals using a high-viscosity injector at APS. The resolution of the crystal structures obtained in this study was dictated by the current flux density and crystal size, but upcoming developments in beamline optics and the planned APS-U upgrade will increase the intensity by two orders of magnitude. These developments will enable structure determination from smaller and/or weakly diffracting microcrystals.

KW - Advanced Photon Source

KW - high-viscosity injector

KW - serial millisecond crystallography

KW - synchrotron radiation

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DO - 10.1107/S205225251700570X

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VL - 4

SP - 439

EP - 454

JO - IUCrJ

JF - IUCrJ

ER -

Serial millisecond crystallography of membrane and soluble protein microcrystals using synchrotron radiation

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