A simple vapor-diffusion method enables protein crystallization inside the HARE 
serial crystallography chip

Norton-Baker, B.; Mehrabi, P.; Boger, J.; Schönherr, R.; von Stetten, D.; Schikora, H.; Kwok, A. O.; Martin, R. W.; Miller, R. J. Dwayne; Redecke, L.; Schulz, E.-C.

doi:10.1107/S2059798321003855

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A simple vapor-diffusion method enables protein crystallization inside the HARE serial crystallography chip

Norton-Baker, B., Mehrabi, P., Boger, J., Schönherr, R., von Stetten, D., Schikora, H., et al. (2021). A simple vapor-diffusion method enables protein crystallization inside the HARE serial crystallography chip. Acta Crystallographica Section D: Structural Biology, 77(6): D77. doi:10.1107/S2059798321003855.

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Supporting information: 3D-Files to re-generate the HARE-chip crystallization tray (txt), Crystal hit-maps (pdf)

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Creators:
Norton-Baker, B.^{1, 2}, Author
Mehrabi, P.^{1, 3}, Author
Boger, J.⁴, Author
Schönherr, R.^{4, 5}, Author
von Stetten, D.⁶, Author
Schikora, H.⁷, Author
Kwok, A. O.², Author
Martin, R. W.^{2, 8}, Author
Miller, R. J. Dwayne^{9, 10}, Author
Redecke, L.^{4, 5}, Author
Schulz, E.-C.^{1, 3}, Author

Affiliations:
1Miller Group, Atomically Resolved Dynamics Department, Max Planck Institute for the Structure and Dynamics of Matter, Max Planck Society, ou_1938288
2Department of Chemistry, University of California, ou_persistent22
3Hamburg Centre for Ultrafast Imaging, Universität Hamburg, ou_persistent22
4Institute of Biochemistry, Center for Structural and Cell Biology in Medicine, University of Lübeck, ou_persistent22
5Photon Science, Deutsches Elektronen-Synchrotron (DESY), ou_persistent22
6European Molecular Biology Laboratory, Hamburg Unit c/o Deutsches Elektronen-Synchrotron, ou_persistent22
7Machine Physics, Scientific Service Units, Max Planck Institute for the Structure and Dynamics of Matter, Max Planck Society, ou_2074322
8Department of Molecular Biology and Biochemistry, University of California, ou_persistent22
9Department of Physics, Universität Hamburg, ou_persistent22
10Departments of Chemistry and Physics, University of Toronto, ou_persistent22

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Free keywords: fixed-target crystallography; serial crystallography; protein crystallization; in cellulo crystallization; in vivo crystals

Abstract: Fixed-target serial crystallography has become an important method for the study of protein structure and dynamics at synchrotrons and X-ray free-electron lasers. However, sample homogeneity, consumption and the physical stress on samples remain major challenges for these high-throughput experiments, which depend on high-quality protein microcrystals. The batch crystallization procedures that are typically applied require time- and sample-intensive screening and optimization. Here, a simple protein crystallization method inside the features of the HARE serial crystallography chips is reported that circumvents batch crystallization and allows the direct transfer of canonical vapor-diffusion conditions to in-chip crystallization. Based on conventional hanging-drop vapor-diffusion experiments, the crystallization solution is distributed into the wells of the HARE chip and equilibrated against a reservoir with mother liquor. Using this simple method, high-quality microcrystals were generated with sufficient density for the structure determination of four different proteins. A new protein variant was crystallized using the protein concentrations encountered during canonical crystallization experiments, enabling structure determination from ∼55 µg of protein. Additionally, structure determination from intracellular crystals grown in insect cells cultured directly in the features of the HARE chips is demonstrated. In cellulo crystallization represents a comparatively unexplored space in crystallization, especially for proteins that are resistant to crystallization using conventional techniques, and eliminates any need for laborious protein purification. This in-chip technique avoids harvesting the sensitive crystals or any further physical handling of the crystal-containing cells. These proof-of-principle experiments indicate the potential of this method to become a simple alternative to batch crystallization approaches and also as a convenient extension to canonical crystallization screens.

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Language(s): eng - English

Dates: Submitted: 2021-02-18Accepted: 2021-04-10Published Online: 2021-05-19

Publication Status: Published online

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Rev. Type: Peer

Identifiers: DOI: 10.1107/S2059798321003855

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Project name : The authors would like to thank Drs A. R. Pearson, M. Agthe, S. Horrell, G. Bourenkov and T. R. Schneider for their continuous support and helpful discussion in the imple- mentation and improvement of these instruments. SSX diffraction data were collected on beamline P14-2 (T-REXX) at the PETRA III storage ring at DESY operated by EMBL Hamburg. Author contributions are as follows. ECS initiated and devised the research. AOK purified -crystallin. BNB carried out in-chip crystallization experiments. HS and ECS designed the in-chip crystallization tray. PM, ECS, JB and DvS carried out data collection and processing. RS, JB and LR carried out all in cellulo experiments. BNB, LR and ECS wrote the manuscript. All authors discussed and corrected the manuscript. Open access funding enabled and organized by Projekt DEAL.

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Title: Acta Crystallographica Section D: Structural Biology

Abbreviation : Acta Cryst. D

Source Genre: Journal

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Publ. Info: Chester, England : International Union of Crystallography

Pages: - Volume / Issue: 77 (6) Sequence Number: D77 Start / End Page: - Identifier: ISSN: 2059-7983
CoNE: https://pure.mpg.de/cone/journals/resource/2059-7983