Your search keyword '"Crystallography, X-Ray methods"' showing total 5,315 results

1. The Importance of Stereochemistry in 5-HT 7 R Modulation─A Case Study of Hydantoin Derivatives.

Author

Kucwaj-Brysz K, Baś S, Żesławska E, Podlewska S, Jastrzębska-Więsek M, Partyka A, Nitek W, Satała G, Wesołowska A, and Handzlik J

Subjects

Animals, Stereoisomerism, Humans, Crystallography, X-Ray methods, Antidepressive Agents pharmacology, Antidepressive Agents chemistry, Mice, Male, Structure-Activity Relationship, Models, Molecular, Receptors, Serotonin metabolism, Receptors, Serotonin drug effects, Hydantoins pharmacology, Hydantoins chemistry, Serotonin Antagonists pharmacology, Serotonin Antagonists chemistry

Abstract

Serotonin 5-HT 7 receptor (5-HT 7 R), one of the most recently discovered members of the serotonergic system, has become a promising target in the search for central nervous system disorders. Despite the number of preclinical results, none of the selective 5-HT 7 R agents has been approved; therefore, the clinical significance of this protein has not been confirmed yet. Recently, we described very promising, selective, and highly potent hydantoin-derived 5-HT 7 R antagonists with confirmed antidepressant activity in vivo and a very good ADMET profile; however, they have been tested in behavioral studies as racemates. In this work, the synthesis of optically pure hydantoin-derived 5-HT 7 R agents using cost-effective, classical methods has been presented for the first time. X-ray crystallographic analysis confirmed the absolute configuration on both stereogenic centers and allowed for the elucidation of the mechanism of introduction of epichlorohydrin into the hydantoin N3-position. The radioligand binding results showed a clear configuration preference for 5-HT 7 R affinity. The molecular modeling results further indicated the key interaction responsible for lower affinity (with amino acid I3 × 29). Finally, the comparison of the antidepressant and anxiolytic effects of racemates versus stereoisomers suggests an influence of additional, apart from the action on 5HT 7 R, factors responsible for the activity in vivo , which is worthy of deeper insight within further studies.

Published

2024

2. Crystal structure of a bacterial photoactivated adenylate cyclase determined by serial femtosecond and serial synchrotron crystallography.

Author

Kapetanaki SM, Coquelle N, von Stetten D, Byrdin M, Rios-Santacruz R, Bean R, Bielecki J, Boudjelida M, Fekete Z, Grime GW, Han H, Hatton C, Kantamneni S, Kharitonov K, Kim C, Kloos M, Koua FHM, de Diego Martinez I, Melo D, Rane L, Round A, Round E, Sarma A, Schubert R, Schulz J, Sikorski M, Vakili M, Valerio J, Vitas J, de Wijn R, Wrona A, Zala N, Pearson A, Dörner K, Schirò G, Garman EF, Lukács A, and Weik M

Subjects

Crystallography, X-Ray methods, Protein Conformation, Oscillatoria enzymology, Flavin-Adenine Dinucleotide metabolism, Flavin-Adenine Dinucleotide chemistry, Models, Molecular, Bacterial Proteins chemistry, Bacterial Proteins genetics, Bacterial Proteins metabolism, Synchrotrons, Adenylyl Cyclases genetics, Adenylyl Cyclases chemistry, Adenylyl Cyclases metabolism

Abstract

OaPAC is a recently discovered blue-light-using flavin adenosine dinucleotide (BLUF) photoactivated adenylate cyclase from the cyanobacterium Oscillatoria acuminata that uses adenosine triphosphate and translates the light signal into the production of cyclic adenosine monophosphate. Here, we report crystal structures of the enzyme in the absence of its natural substrate determined from room-temperature serial crystallography data collected at both an X-ray free-electron laser and a synchrotron, and we compare these structures with cryo-macromolecular crystallography structures obtained at a synchrotron by us and others. These results reveal slight differences in the structure of the enzyme due to data collection at different temperatures and X-ray sources. We further investigate the effect of the Y6W mutation in the BLUF domain, a mutation which results in a rearrangement of the hydrogen-bond network around the flavin and a notable rotation of the side chain of the critical Gln48 residue. These studies pave the way for picosecond-millisecond time-resolved serial crystallography experiments at X-ray free-electron lasers and synchrotrons in order to determine the early structural intermediates and correlate them with the well studied picosecond-millisecond spectroscopic intermediates., (open access.)

Published

2024

3. Analysis of crystallographic phase retrieval using iterative projection algorithms.

Author

Barnett MJ, Millane RP, and Kingston RL

Subjects

Crystallography, X-Ray methods, Protein Conformation, Models, Molecular, Algorithms, Proteins chemistry

Abstract

For protein crystals in which more than two thirds of the volume is occupied by solvent, the featureless nature of the solvent region often generates a constraint that is powerful enough to allow direct phasing of X-ray diffraction data. Practical implementation relies on the use of iterative projection algorithms with good global convergence properties to solve the difficult nonconvex phase-retrieval problem. In this paper, some aspects of phase retrieval using iterative projection algorithms are systematically explored, where the diffraction data and density-value distributions in the protein and solvent regions provide the sole constraints. The analysis is based on the addition of random error to the phases of previously determined protein crystal structures, followed by evaluation of the ability to recover the correct phase set as the distance from the solution increases. The properties of the difference-map (DM), relaxed-reflect-reflect (RRR) and relaxed averaged alternating reflectors (RAAR) algorithms are compared. All of these algorithms prove to be effective for crystallographic phase retrieval, and the useful ranges of the adjustable parameter which controls their behavior are established. When these algorithms converge to the solution, the algorithm trajectory becomes stationary; however, the density function continues to fluctuate significantly around its mean position. It is shown that averaging over the algorithm trajectory in the stationary region, following convergence, improves the density estimate, with this procedure outperforming previous approaches for phase or density refinement., (open access.)

Published

2024

4. Improving the diffraction quality of heat-shock protein 47 crystals.

Author

Kish K, Cobell S, Szapiel N, Yan C, Newitt JA, Tredup J, Rodrigo I, Tomasco E, Gao M, Marsilio F, Haugner J, Lipovšek D, Deng B, Bousquet P, Zhang Y, Schmidt H, and Sheriff S

Subjects

Animals, Crystallography, X-Ray methods, Dogs, Humans, Models, Molecular, Escherichia coli metabolism, Escherichia coli genetics, Fibronectins chemistry, Fibronectins metabolism, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Gene Expression, HSP47 Heat-Shock Proteins chemistry, HSP47 Heat-Shock Proteins metabolism, HSP47 Heat-Shock Proteins genetics, Crystallization

Abstract

Heat-shock protein 47 (HSP47) is a potential target for inhibitors that ameliorate fibrosis by reducing collagen assembly. In an effort to develop a structure-based drug-design system, it was not possible to replicate a previous literature result (PDB entry 4au4) for apo dog HSP47; instead, crystal forms were obtained in which pairs of dog HSP47 molecules interacted through a noncleavable C-terminal His-tag to build up tetramers, all of which had multiple molecules of HSP47 in the asymmetric unit and none of which diffracted as well as the literature precedent. To overcome these difficulties, a two-pronged approach was followed: (i) the His-tag was moved from the C-terminus to the N-terminus and was made cleavable, and (ii) Adnectin (derived from the tenth domain of human fibronectin type III) crystallization chaperones were developed. Both approaches provided well diffracting crystals, but the latter approach yielded crystal forms with only one or two HSP47 complexes per asymmetric unit, which made model building less onerous.

Published

2024

5. De novo protein design with a denoising diffusion network independent of pretrained structure prediction models.

Author

Liu Y, Wang S, Dong J, Chen L, Wang X, Wang L, Li F, Wang C, Zhang J, Wang Y, Wei S, Chen Q, and Liu H

Subjects

Protein Conformation, Models, Molecular, Algorithms, Protein Folding, Models, Statistical, Computational Biology methods, Crystallography, X-Ray methods, Proteins chemistry

Abstract

The recent success of RFdiffusion, a method for protein structure design with a denoising diffusion probabilistic model, has relied on fine-tuning the RoseTTAFold structure prediction network for protein backbone denoising. Here, we introduce SCUBA-diffusion (SCUBA-D), a protein backbone denoising diffusion probabilistic model freshly trained by considering co-diffusion of sequence representation to enhance model regularization and adversarial losses to minimize data-out-of-distribution errors. While matching the performance of the pretrained RoseTTAFold-based RFdiffusion in generating experimentally realizable protein structures, SCUBA-D readily generates protein structures with not-yet-observed overall folds that are different from those predictable with RoseTTAFold. The accuracy of SCUBA-D was confirmed by the X-ray structures of 16 designed proteins and a protein complex, and by experiments validating designed heme-binding proteins and Ras-binding proteins. Our work shows that deep generative models of images or texts can be fruitfully extended to complex physical objects like protein structures by addressing outstanding issues such as the data-out-of-distribution errors., (© 2024. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2024

6. The success rate of processed predicted models in molecular replacement: implications for experimental phasing in the AlphaFold era.

Author

Keegan RM, Simpkin AJ, and Rigden DJ

Subjects

Crystallography, X-Ray methods, Databases, Protein, Software, Protein Folding, Models, Molecular, Proteins chemistry, Protein Conformation

Abstract

The availability of highly accurate protein structure predictions from AlphaFold2 (AF2) and similar tools has hugely expanded the applicability of molecular replacement (MR) for crystal structure solution. Many structures can be solved routinely using raw models, structures processed to remove unreliable parts or models split into distinct structural units. There is therefore an open question around how many and which cases still require experimental phasing methods such as single-wavelength anomalous diffraction (SAD). Here, this question is addressed using a large set of PDB depositions that were solved by SAD. A large majority (87%) could be solved using unedited or minimally edited AF2 predictions. A further 18 (4%) yield straightforwardly to MR after splitting of the AF2 prediction using Slice'N'Dice, although different splitting methods succeeded on slightly different sets of cases. It is also found that further unique targets can be solved by alternative modelling approaches such as ESMFold (four cases), alternative MR approaches such as ARCIMBOLDO and AMPLE (two cases each), and multimeric model building with AlphaFold-Multimer or UniFold (three cases). Ultimately, only 12 cases, or 3% of the SAD-phased set, did not yield to any form of MR tested here, offering valuable hints as to the number and the characteristics of cases where experimental phasing remains essential for macromolecular structure solution., (open access.)

Published

2024

7. Establishing Composition of Solid Solution Based on Single Crystal and Powder X-ray Measurement: The Case of Halogenated Bismuth(III) Complexes with Acetophenone-4-methyl-3-thiosemicarbazone.

Author

Grześkiewicz AM, Dutkiewicz G, Ozturk II, and Kubicki M

Subjects

Crystallography, X-Ray methods, Acetophenones chemistry, Halogenation, Models, Molecular, Molecular Structure, Powder Diffraction, X-Ray Diffraction methods, Thiosemicarbazones chemistry, Bismuth chemistry, Coordination Complexes chemistry

Abstract

New bismuth (III) complexes with acetophenone-4-methyl-3-thiosemicarbazone (L) and halogens (Cl and Br) in both bridging and terminal positions have been synthesized and structurally characterized using single-crystal X-ray diffraction. The pure complexes (Cl or Br) were found to be highly isostructural, which motivated our attempts to create solid solutions of these complexes. A series of such compounds was prepared using various procedures and stoichiometries. A method for determining the mutual concentrations of different halogens, based on the positions of selected peaks in powder diffraction patterns, was tested and compared with other methods.

Published

2024

8. Robust and automatic beamstop shadow outlier rejection: combining crystallographic statistics with modern clustering under a semi-supervised learning strategy.

Author

Gao Y, Ginn HM, and Thorn A

Subjects

Crystallography, X-Ray methods, Cluster Analysis, Supervised Machine Learning, Algorithms

Abstract

During the automatic processing of crystallographic diffraction experiments, beamstop shadows are often unaccounted for or only partially masked. As a result of this, outlier reflection intensities are integrated, which is a known issue. Traditional statistical diagnostics have only limited effectiveness in identifying these outliers, here termed Not-Excluded-unMasked-Outliers (NEMOs). The diagnostic tool AUSPEX allows visual inspection of NEMOs, where they form a typical pattern: clusters at the low-resolution end of the AUSPEX plots of intensities or amplitudes versus resolution. To automate NEMO detection, a new algorithm was developed by combining data statistics with a density-based clustering method. This approach demonstrates a promising performance in detecting NEMOs in merged data sets without disrupting existing data-reduction pipelines. Re-refinement results indicate that excluding the identified NEMOs can effectively enhance the quality of subsequent structure-determination steps. This method offers a prospective automated means to assess the efficacy of a beamstop mask, as well as highlighting the potential of modern pattern-recognition techniques for automating outlier exclusion during data processing, facilitating future adaptation to evolving experimental strategies., (open access.)

Published

2024

9. CHiMP: deep-learning tools trained on protein crystallization micrographs to enable automation of experiments.

Author

King ONF, Levik KE, Sandy J, and Basham M

Subjects

Crystallography, X-Ray methods, Proteins chemistry, Image Processing, Computer-Assisted methods, Synchrotrons, Automation, Software, Deep Learning, Crystallization methods

Abstract

A group of three deep-learning tools, referred to collectively as CHiMP (Crystal Hits in My Plate), were created for analysis of micrographs of protein crystallization experiments at the Diamond Light Source (DLS) synchrotron, UK. The first tool, a classification network, assigns images into categories relating to experimental outcomes. The other two tools are networks that perform both object detection and instance segmentation, resulting in masks of individual crystals in the first case and masks of crystallization droplets in addition to crystals in the second case, allowing the positions and sizes of these entities to be recorded. The creation of these tools used transfer learning, where weights from a pre-trained deep-learning network were used as a starting point and repurposed by further training on a relatively small set of data. Two of the tools are now integrated at the VMXi macromolecular crystallography beamline at DLS, where they have the potential to absolve the need for any user input, both for monitoring crystallization experiments and for triggering in situ data collections. The third is being integrated into the XChem fragment-based drug-discovery screening platform, also at DLS, to allow the automatic targeting of acoustic compound dispensing into crystallization droplets., (open access.)

Published

2024

10. Utilizing anomalous signals for element identification in macromolecular crystallography.

Author

El Omari K, Forsyth I, Duman R, Orr CM, Mykhaylyk V, Mancini EJ, and Wagner A

Subjects

Crystallography, X-Ray methods, Protein Conformation, Macromolecular Substances chemistry, Metals chemistry, Models, Molecular, Proteins chemistry

Abstract

AlphaFold2 has revolutionized structural biology by offering unparalleled accuracy in predicting protein structures. Traditional methods for determining protein structures, such as X-ray crystallography and cryo-electron microscopy, are often time-consuming and resource-intensive. AlphaFold2 provides models that are valuable for molecular replacement, aiding in model building and docking into electron density or potential maps. However, despite its capabilities, models from AlphaFold2 do not consistently match the accuracy of experimentally determined structures, need to be validated experimentally and currently miss some crucial information, such as post-translational modifications, ligands and bound ions. In this paper, the advantages are explored of collecting X-ray anomalous data to identify chemical elements, such as metal ions, which are key to understanding certain structures and functions of proteins. This is achieved through methods such as calculating anomalous difference Fourier maps or refining the imaginary component of the anomalous scattering factor f''. Anomalous data can serve as a valuable complement to the information provided by AlphaFold2 models and this is particularly significant in elucidating the roles of metal ions., (open access.)

Published

2024

11. Insights into the structure and activation mechanism of some class B1 GPCR family members.

Author

Aksu H, Demirbilek A, and Uba AI

Subjects

Humans, Crystallography, X-Ray methods, Protein Conformation, Animals, Glucagon-Like Peptide-1 Receptor metabolism, Glucagon-Like Peptide-1 Receptor genetics, Receptors, Gastrointestinal Hormone metabolism, Receptors, Gastrointestinal Hormone chemistry, Receptors, Gastrointestinal Hormone genetics, Glucagon-Like Peptide 1 metabolism, Models, Molecular, Protein Binding, Signal Transduction, Receptors, Glucagon metabolism, Receptors, Glucagon genetics, Receptors, Glucagon chemistry, Receptors, G-Protein-Coupled metabolism, Receptors, G-Protein-Coupled chemistry, Receptors, G-Protein-Coupled genetics

Abstract

In humans, 15 genes encode the class B1 family of GPCRs, which are polypeptide hormone receptors characterized by having a large N-terminal extracellular domain (ECD) and receive signals from outside the cell to activate cellular response. For example, the insulinotropic polypeptide (GIP) stimulates the glucose-dependent insulinotropic polypeptide receptor (GIPR), while the glucagon receptor (GCGR) responds to glucagon by increasing blood glucose levels and promoting the breakdown of liver glycogen to induce the production of insulin. The glucagon-like peptides 1 and 2 (GLP-1 and GLP-2) elicit a response from glucagon-like peptide receptor types 1 and 2 (GLP1R and GLP2R), respectively. Since these receptors are implicated in the pathogenesis of diabetes, studying their activation is crucial for the development of effective therapies for the condition. With more structural information being revealed by experimental methods such as X-ray crystallography, cryo-EM, and NMR, the activation mechanism of class B1 GPCRs becomes unraveled. The available crystal and cryo-EM structures reveal that class B1 GPCRs follow a two-step model for peptide binding and receptor activation. The regions close to the C-termini of hormones interact with the N-terminal ECD of the receptor while the regions close to the N-terminus of the peptide interact with the TM domain and transmit signals. This review highlights the structural details of class B1 GPCRs and their conformational changes following activation. The roles of MD simulation in characterizing those conformational changes are briefly discussed, providing insights into the potential structural exploration for future ligand designs., (© 2024. The Author(s), under exclusive licence to Springer Nature B.V.)

Published

2024

12. 19 F NMR Reveals the Dynamics of Substrate Binding and Lid Closure for Iodotyrosine Deiodinase as a Complement to Steady-State Kinetics and Crystallography.

Author

Greenberg HC, Majumdar A, Cheema EK, Kozyryev A, and Rokita SE

Subjects

Kinetics, Crystallography, X-Ray methods, Nuclear Magnetic Resonance, Biomolecular, Protein Conformation, Substrate Specificity, Humans, Fluorine chemistry, Fluorine metabolism, Models, Molecular, Protein Binding, Ligands, Iodide Peroxidase metabolism, Iodide Peroxidase chemistry, Catalytic Domain

Abstract

Active site lids are common features of enzymes and typically undergo conformational changes upon substrate binding to promote catalysis. Iodotyrosine deiodinase is no exception and contains a lid segment in all of its homologues from human to bacteria. The solution-state dynamics of the lid have now been characterized using 19 F NMR spectroscopy with a CF 3 -labeled enzyme and CF 3 O-labeled ligands. From two-dimensional 19 F- 19 F NMR exchange spectroscopy, interconversion rates between the free and bound states of a CF 3 O-substituted tyrosine (45 ± 10 s -1 ) and the protein label (40 ± 3 s -1 ) are very similar and suggest a correlation between ligand binding and conformational reorganization of the lid. Both occur at rates that are ∼100-fold faster than turnover, and therefore these steps do not limit catalysis. A simple CF 3 O-labeled phenol also binds to the active site and induces a conformational change in the lid segment that was not previously detectable by crystallography. Exchange rates of the ligand (130 ± 20 s -1 ) and protein (98 ± 8 s -1 ) in this example are faster than those above but remain self-consistent to affirm a correlation between ordering of the lid and binding of the ligand. Both ligands also protect the protein from limited proteolysis, as expected from their ability to stabilize a compact lid structure. However, the minimal turnover of simple phenol substrates indicates that such stabilization may be necessary but is not sufficient for efficient catalysis.

Published

2024

13. Microcrystal electron diffraction structure of Toll-like receptor 2 TIR-domain-nucleated MyD88 TIR-domain higher-order assembly.

Author

Li Y, Pacoste LC, Gu W, Thygesen SJ, Stacey KJ, Ve T, Kobe B, Xu H, and Nanson JD

Subjects

Humans, Protein Domains, Models, Molecular, Toll-Like Receptor 6 chemistry, Toll-Like Receptor 6 metabolism, Toll-Like Receptor 1 chemistry, Toll-Like Receptor 1 metabolism, Crystallography, X-Ray methods, Receptors, Interleukin-1 chemistry, Receptors, Interleukin-1 metabolism, Protein Multimerization, Toll-Like Receptor 2 chemistry, Toll-Like Receptor 2 metabolism, Myeloid Differentiation Factor 88 chemistry, Myeloid Differentiation Factor 88 metabolism

Abstract

Eukaryotic TIR (Toll/interleukin-1 receptor protein) domains signal via TIR-TIR interactions, either by self-association or by interaction with other TIR domains. In mammals, TIR domains are found in Toll-like receptors (TLRs) and cytoplasmic adaptor proteins involved in pro-inflammatory signaling. Previous work revealed that the MAL TIR domain (MAL TIR ) nucleates the assembly of MyD88 TIR into crystalline arrays in vitro. A microcrystal electron diffraction (MicroED) structure of the MyD88 TIR assembly has previously been solved, revealing a two-stranded higher-order assembly of TIR domains. In this work, it is demonstrated that the TIR domain of TLR2, which is reported to signal as a heterodimer with either TLR1 or TLR6, induces the formation of crystalline higher-order assemblies of MyD88 TIR in vitro, whereas TLR1 TIR and TLR6 TIR do not. Using an improved data-collection protocol, the MicroED structure of TLR2 TIR -induced MyD88 TIR microcrystals was determined at a higher resolution (2.85 Å) and with higher completeness (89%) compared with the previous structure of the MAL TIR -induced MyD88 TIR assembly. Both assemblies exhibit conformational differences in several areas that are important for signaling (for example the BB loop and CD loop) compared with their monomeric structures. These data suggest that TLR2 TIR and MAL TIR interact with MyD88 in an analogous manner during signaling, nucleating MyD88 TIR assemblies unidirectionally., (open access.)

Published

2024

14. The structure of Chlamydomonas LOV1 as revealed by time-resolved serial synchrotron crystallography.

Author

Schmidt M

Subjects

Crystallography, X-Ray methods, Models, Molecular, Flavin Mononucleotide chemistry, Protein Domains, Chlamydomonas chemistry, Chlamydomonas metabolism, Chlamydomonas reinhardtii chemistry, Chlamydomonas reinhardtii metabolism, Phototropins chemistry, Phototropins metabolism, Synchrotrons

Abstract

The photo-reaction of the LOV1 domain of the Chlamydomonas reinhardtii phototropin is investigated by room-temperature time-resolved serial crystallography. A covalent adduct forms between the C4a atom of the central flavin-mononucleotide chromophore and a protein cysteine. The structure of the adduct is very similar to that of LOV2 determined 23 years ago from the maidenhair fern Phy3., (open access.)

Published

2024

15. Surface-mutagenesis strategies to enable structural biology crystallization platforms.

Author

Schaefer M, Pütter V, Hilpmann A, Egner U, Holton SJ, and Hillig RC

Subjects

Crystallography, X-Ray methods, Humans, Drug Discovery methods, Mutation, Models, Molecular, Protein Serine-Threonine Kinases chemistry, Crystallization methods

Abstract

A key prerequisite for the successful application of protein crystallography in drug discovery is to establish a robust crystallization system for a new drug-target protein fast enough to deliver crystal structures when the first inhibitors have been identified in the hit-finding campaign or, at the latest, in the subsequent hit-to-lead process. The first crucial step towards generating well folded proteins with a high likelihood of crystallizing is the identification of suitable truncation variants of the target protein. In some cases an optimal length variant alone is not sufficient to support crystallization and additional surface mutations need to be introduced to obtain suitable crystals. In this contribution, four case studies are presented in which rationally designed surface modifications were key to establishing crystallization conditions for the target proteins (the protein kinases Aurora-C, IRAK4 and BUB1, and the KRAS-SOS1 complex). The design process which led to well diffracting crystals is described and the crystal packing is analysed to understand retrospectively how the specific surface mutations promoted successful crystallization. The presented design approaches are routinely used in our team to support the establishment of robust crystallization systems which enable structure-guided inhibitor optimization for hit-to-lead and lead-optimization projects in pharmaceutical research., (open access.)

Published

2024

16. Comparison of two crystal polymorphs of NowGFP reveals a new conformational state trapped by crystal packing.

Author

Kim JK, Jeong H, Seo J, Kim S, Kim KH, Min D, and Kim CU

Subjects

Crystallography, X-Ray methods, Crystallization, Green Fluorescent Proteins chemistry, Protein Conformation, Models, Molecular

Abstract

Crystal polymorphism serves as a strategy to study the conformational flexibility of proteins. However, the relationship between protein crystal packing and protein conformation often remains elusive. In this study, two distinct crystal forms of a green fluorescent protein variant, NowGFP, are compared: a previously identified monoclinic form (space group C2) and a newly discovered orthorhombic form (space group P2 1 2 1 2 1 ). Comparative analysis reveals that both crystal forms exhibit nearly identical linear assemblies of NowGFP molecules interconnected through similar crystal contacts. However, a notable difference lies in the stacking of these assemblies: parallel in the monoclinic form and perpendicular in the orthorhombic form. This distinct mode of stacking leads to different crystal contacts and induces structural alteration in one of the two molecules within the asymmetric unit of the orthorhombic crystal form. This new conformational state captured by orthorhombic crystal packing exhibits two unique features: a conformational shift of the β-barrel scaffold and a restriction of pH-dependent shifts of the key residue Lys61, which is crucial for the pH-dependent spectral shift of this protein. These findings demonstrate a clear connection between crystal packing and alternative conformational states of proteins, providing insights into how structural variations influence the function of fluorescent proteins., (open access.)

Published

2024

17. Mechanistic Insights from the Crystal Structure and Computational Analysis of the Radical SAM Deaminase DesII.

Author

Hou X, Feng J, Franklin JL, Russo R, Guo Z, Zhou J, Gao JM, Liu HW, and Wang B

Subjects

Crystallography, X-Ray methods, Models, Molecular, S-Adenosylmethionine metabolism, S-Adenosylmethionine chemistry, Catalytic Domain, Bacterial Proteins, Streptomyces enzymology

Abstract

Radical S-adenosyl-L-methionine (SAM) enzymes couple the reductive cleavage of SAM to radical-mediated transformations that have proven to be quite broad in scope. DesII is one such enzyme from the biosynthetic pathway of TDP-desosamine where it catalyzes a radical-mediated deamination. Previous studies have suggested that this reaction proceeds via direct elimination of ammonia from an α-hydroxyalkyl radical or its conjugate base (i.e., a ketyl radical) rather than 1,2-migration of the amino group to form a carbinolamine radical intermediate. However, without a crystal structure, the active site features responsible for this chemistry have remained largely unknown. The crystallographic studies described herein help to fill this gap by providing a structural description of the DesII active site. Computational analyses based on the solved crystal structure are consistent with direct elimination and indicate that an active site glutamate residue likely serves as a general base to promote deprotonation of the α-hydroxyalkyl radical intermediate and elimination of the ammonia group., (© 2024 The Author(s). Advanced Science published by Wiley‐VCH GmbH.)

Published

2024

18. CheckMyMetal (CMM): validating metal-binding sites in X-ray and cryo-EM data.

Author

Gucwa M, Bijak V, Zheng H, Murzyn K, and Minor W

Subjects

Binding Sites, RNA, Transfer chemistry, Ribosomes chemistry, Crystallography, X-Ray methods, Metals chemistry

Abstract

Identifying and characterizing metal-binding sites (MBS) within macromolecular structures is imperative for elucidating their biological functions. CheckMyMetal (CMM) is a web based tool that facilitates the interactive validation of MBS in structures determined through X-ray crystallography and cryo-electron microscopy (cryo-EM). Recent updates to CMM have significantly enhanced its capability to efficiently handle large datasets generated from cryo-EM structural analyses. In this study, we address various challenges inherent in validating MBS within both X-ray and cryo-EM structures. Specifically, we examine the difficulties associated with accurately identifying metals and modeling their coordination environments by considering the ongoing reproducibility challenges in structural biology and the critical importance of well annotated, high-quality experimental data. CMM employs a sophisticated framework of rules rooted in the valence bond theory for MBS validation. We explore how CMM validation parameters correlate with the resolution of experimentally derived structures of macromolecules and their complexes. Additionally, we showcase the practical utility of CMM by analyzing a representative cryo-EM structure. Through a comprehensive examination of experimental data, we demonstrate the capability of CMM to advance MBS characterization and identify potential instances of metal misassignment., (open access.)

Published

2024

19. Exploring serial crystallography for drug discovery.

Author

Dunge A, Phan C, Uwangue O, Bjelcic M, Gunnarsson J, Wehlander G, Käck H, and Brändén G

Subjects

Crystallography, X-Ray methods, Protein Conformation, Ligands, Humans, Temperature, Models, Molecular, Crystallography methods, Crystallization, Drug Discovery methods, Epoxide Hydrolases chemistry, Epoxide Hydrolases antagonists & inhibitors, Epoxide Hydrolases metabolism

Abstract

Structure-based drug design is highly dependent on the availability of structures of the protein of interest in complex with lead compounds. Ideally, this information can be used to guide the chemical optimization of a compound into a pharmaceutical drug candidate. A limitation of the main structural method used today - conventional X-ray crystallography - is that it only provides structural information about the protein complex in its frozen state. Serial crystallography is a relatively new approach that offers the possibility to study protein structures at room temperature (RT). Here, we explore the use of serial crystallography to determine the structures of the pharmaceutical target, soluble epoxide hydrolase. We introduce a new method to screen for optimal microcrystallization conditions suitable for use in serial crystallography and present a number of RT ligand-bound structures of our target protein. From a comparison between the RT structural data and previously published cryo-temperature structures, we describe an example of a temperature-dependent difference in the ligand-binding mode and observe that flexible loops are better resolved at RT. Finally, we discuss the current limitations and potential future advances of serial crystallography for use within pharmaceutical drug discovery., (open access.)

Published

2024

20. In situ serial crystallography facilitates 96-well plate structural analysis at low symmetry.

Author

Foos N, Florial JB, Eymery M, Sinoir J, Felisaz F, Oscarsson M, Beteva A, Bowler MW, Nurizzo D, Papp G, Soler-Lopez M, Nanao M, Basu S, and McCarthy AA

Subjects

Crystallography, X-Ray methods, Humans, Protein Conformation, Synchrotrons, Crystallization

Abstract

The advent of serial crystallography has rejuvenated and popularized room-temperature X-ray crystal structure determination. Structures determined at physiological temperature reveal protein flexibility and dynamics. In addition, challenging samples (e.g. large complexes, membrane proteins and viruses) form fragile crystals that are often difficult to harvest for cryo-crystallography. Moreover, a typical serial crystallography experiment requires a large number of microcrystals, mainly achievable through batch crystallization. Many medically relevant samples are expressed in mammalian cell lines, producing a meager quantity of protein that is incompatible with batch crystallization. This can limit the scope of serial crystallography approaches. Direct in situ data collection from a 96-well crystallization plate enables not only the identification of the best diffracting crystallization condition but also the possibility for structure determination under ambient conditions. Here, we describe an in situ serial crystallography (iSX) approach, facilitating direct measurement from crystallization plates mounted on a rapidly exchangeable universal plate holder deployed at a microfocus beamline, ID23-2, at the European Synchrotron Radiation Facility. We applied our iSX approach on a challenging project, autotaxin, a therapeutic target expressed in a stable human cell line, to determine the structure in the lowest-symmetry P1 space group at 3.0 Å resolution. Our in situ data collection strategy provided a complete dataset for structure determination while screening various crystallization conditions. Our data analysis reveals that the iSX approach is highly efficient at a microfocus beamline, improving throughput and demonstrating how crystallization plates can be routinely used as an alternative method of presenting samples for serial crystallography experiments at synchrotrons., (open access.)

Published

2024

21. Capturing the blue-light activated state of the Phot-LOV1 domain from Chlamydomonas reinhardtii using time-resolved serial synchrotron crystallography.

Author

Gotthard G, Mous S, Weinert T, Maia RNA, James D, Dworkowski F, Gashi D, Furrer A, Ozerov D, Panepucci E, Wang M, Schertler GFX, Heberle J, Standfuss J, and Nogly P

Subjects

Crystallography, X-Ray methods, Light, Phototropins chemistry, Phototropins metabolism, Phototropins genetics, Protein Domains, Chlamydomonas reinhardtii metabolism, Chlamydomonas reinhardtii chemistry, Synchrotrons

Abstract

Light-oxygen-voltage (LOV) domains are small photosensory flavoprotein modules that allow the conversion of external stimuli (sunlight) into intracellular signals responsible for various cell behaviors (e.g. phototropism and chloroplast relocation). This ability relies on the light-induced formation of a covalent thioether adduct between a flavin chromophore and a reactive cysteine from the protein environment, which triggers a cascade of structural changes that result in the activation of a serine/threonine (Ser/Thr) kinase. Recent developments in time-resolved crystallography may allow the activation cascade of the LOV domain to be observed in real time, which has been elusive. In this study, we report a robust protocol for the production and stable delivery of microcrystals of the LOV domain of phototropin Phot-1 from Chlamydomonas reinhardtii (CrPhotLOV1) with a high-viscosity injector for time-resolved serial synchrotron crystallography (TR-SSX). The detailed process covers all aspects, from sample optimization to data collection, which may serve as a guide for soluble protein preparation for TR-SSX. In addition, we show that the crystals obtained preserve the photoreactivity using infrared spectroscopy. Furthermore, the results of the TR-SSX experiment provide high-resolution insights into structural alterations of CrPhotLOV1 from Δt = 2.5 ms up to Δt = 95 ms post-photoactivation, including resolving the geometry of the thioether adduct and the C-terminal region implicated in the signal transduction process., (open access.)

Published

2024

22. IHMCIF: An Extension of the PDBx/mmCIF Data Standard for Integrative Structure Determination Methods.

Author

Vallat B, Webb BM, Westbrook JD, Goddard TD, Hanke CA, Graziadei A, Peisach E, Zalevsky A, Sagendorf J, Tangmunarunkit H, Voinea S, Sekharan M, Yu J, Bonvin AAMJJ, DiMaio F, Hummer G, Meiler J, Tajkhorshid E, Ferrin TE, Lawson CL, Leitner A, Rappsilber J, Seidel CAM, Jeffries CM, Burley SK, Hoch JC, Kurisu G, Morris K, Patwardhan A, Velankar S, Schwede T, Trewhella J, Kesselman C, Berman HM, and Sali A

Subjects

Protein Conformation, Models, Molecular, Software, Crystallography, X-Ray methods, Macromolecular Substances chemistry, Computational Biology methods, Ligands, Databases, Protein, Proteins chemistry

Abstract

IHMCIF (github.com/ihmwg/IHMCIF) is a data information framework that supports archiving and disseminating macromolecular structures determined by integrative or hybrid modeling (IHM), and making them Findable, Accessible, Interoperable, and Reusable (FAIR). IHMCIF is an extension of the Protein Data Bank Exchange/macromolecular Crystallographic Information Framework (PDBx/mmCIF) that serves as the framework for the Protein Data Bank (PDB) to archive experimentally determined atomic structures of biological macromolecules and their complexes with one another and small molecule ligands (e.g., enzyme cofactors and drugs). IHMCIF serves as the foundational data standard for the PDB-Dev prototype system, developed for archiving and disseminating integrative structures. It utilizes a flexible data representation to describe integrative structures that span multiple spatiotemporal scales and structural states with definitions for restraints from a variety of experimental methods contributing to integrative structural biology. The IHMCIF extension was created with the benefit of considerable community input and recommendations gathered by the Worldwide Protein Data Bank (wwPDB) Task Force for Integrative or Hybrid Methods (wwpdb.org/task/hybrid). Herein, we describe the development of IHMCIF to support evolving methodologies and ongoing advancements in integrative structural biology. Ultimately, IHMCIF will facilitate the unification of PDB-Dev data and tools with the PDB archive so that integrative structures can be archived and disseminated through PDB., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2024

23. Crystallographic fragment screen of the c-di-AMP-synthesizing enzyme CdaA from Bacillus subtilis.

Author

Garbers T, Neumann P, Wollenhaupt J, Dickmanns A, Weiss MS, and Ficner R

Subjects

Crystallography, X-Ray methods, Catalytic Domain, Models, Molecular, Dinucleoside Phosphates chemistry, Dinucleoside Phosphates metabolism, Streptococcus pneumoniae enzymology, Streptococcus pneumoniae chemistry, Amino Acid Sequence, Protein Binding, Crystallization, Bacillus subtilis enzymology, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Bacterial Proteins genetics

Abstract

Crystallographic fragment screening has become a pivotal technique in structure-based drug design, particularly for bacterial targets with a crucial role in infectious disease mechanisms. The enzyme CdaA, which synthesizes an essential second messenger cyclic di-AMP (c-di-AMP) in many pathogenic bacteria, has emerged as a promising candidate for the development of novel antibiotics. To identify crystals suitable for fragment screening, CdaA enzymes from Streptococcus pneumoniae, Bacillus subtilis and Enterococcus faecium were purified and crystallized. Crystals of B. subtilis CdaA, which diffracted to the highest resolution of 1.1 Å, were used to perform the screening of 96 fragments, yielding data sets with resolutions spanning from 1.08 to 1.87 Å. A total of 24 structural hits across eight different sites were identified. Four fragments bind to regions that are highly conserved among pathogenic bacteria, specifically the active site (three fragments) and the dimerization interface (one fragment). The coordinates of the three active-site fragments were used to perform an in silico drug-repurposing screen using the OpenEye suite and the DrugBank database. This screen identified tenofovir, an approved drug, that is predicted to interact with the ATP-binding region of CdaA. Its inhibitory potential against pathogenic E. faecium CdaA has been confirmed by ITC measurements. These findings not only demonstrate the feasibility of this approach for identifying lead compounds for the design of novel antibacterial agents, but also pave the way for further fragment-based lead-optimization efforts targeting CdaA., (open access.)

Published

2024

24. Strategy for improving circular dichroism spectra deconvolution accuracy for macrocyclic peptides in drug discovery.

Author

Guo W, Makarov AA, Buevich AV, and Jiang Y

Subjects

Calibration, Magnetic Resonance Spectroscopy methods, Crystallography, X-Ray methods, Circular Dichroism methods, Drug Discovery methods, Peptides, Cyclic chemistry, Protein Structure, Secondary

Abstract

Peptide therapeutics have emerged as an appealing modality in the pharmaceutical industry. Understanding peptide conformation in solution remains one of the most critical areas for peptide drug development. Circular dichroism (CD) spectroscopy is a useful technique to study the secondary structure of proteins and peptides, but the current approaches are limited to protein-focused models to predict high-order structures of peptides, and the models were built based on X-ray crystallography instead of solution-based technique, as a result, such models may have poor predictions for peptides. In this study, we present a novel CD deconvolution model to determine peptide conformation in solution. To quantitatively obtain secondary structure information using CD, a calibration model is needed beforehand to establish the relationship between each secondary structure feature and the corresponding CD response. A reference set containing the majority of cyclic peptides with known structures from solution-state NMR spectroscopy was used to build the calibration model for CD deconvolution. Improved prediction accuracy on the secondary structure determination for cyclic peptides was achieved by this model compared to the commercial standard model using commercially available platforms. This new CD deconvolution method is crucial for peptide conformational analysis in solution, and has the potential to greatly accelerate peptide drug candidate optimization in the pharmaceutical drug discovery field., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2025

25. Wheldone Revisited: Structure Revision Via DFT-GIAO Chemical Shift Calculations, 1,1-HD-ADEQUATE NMR Spectroscopy, and X-ray Crystallography Studies.

Author

Rangel-Grimaldo M, Earp CE, Raja HA, Wood JS, Mardiana L, Ho KL, Longcake A, Williamson RT, Palatinus L, Hall MJ, Probert MR, and Oberlies NH

Subjects

Crystallography, X-Ray methods, Molecular Structure, Aspergillus chemistry, Xylariales chemistry, Humans, Magnetic Resonance Spectroscopy methods

Abstract

Wheldone is a fungal metabolite isolated from the coculture of Aspergillus fischeri and Xylaria flabelliformis , displaying cytotoxic activity against breast, melanoma, and ovarian cancer cell lines. Initially, its structure was characterized as an unusual 5-methyl-bicyclo[5.4.0]undeca-3,5-diene scaffold with a 2-hydroxy-1-propanone side chain and a 3-(2-(1-hydroxyethyl)-2-methyl-2,5-dihydrofuran-3-yl)acrylic acid moiety. Upon further examination, minor inconsistencies in the data suggested the need for the structure to be revisited. Thus, the structure of wheldone has been revised using an orthogonal experimental-computational approach, which combines 1,1-HD-ADEQUATE NMR experiments, DFT-GIAO chemical shift calculations, and single-crystal X-ray diffraction (SCXRD) analysis of a semisynthetic p- bromobenzylamide derivative, formed via a Steglich-type reaction. The summation of these data now permits the unequivocal assignment of both the structure and absolute configuration of the natural product.

Published

2024

26. Variable temperature-nuclear magnetic resonance experiment and high-resolution MS/MS n measurement of hydroxycarbodenafil, and its PDE5 inhibitory activity.

Author

Tachikawa H, Nishiyama R, Kosugi Y, Ichikawa-Kaji Y, Uemura N, Moriuchi Y, Moriyasu T, Suzuki T, and Inomata A

Subjects

Crystallography, X-Ray methods, Tandem Mass Spectrometry methods, Cyclic Nucleotide Phosphodiesterases, Type 5 metabolism, Cyclic Nucleotide Phosphodiesterases, Type 5 chemistry, Piperazines chemistry, Piperazines pharmacology, Piperazines analysis, Phosphodiesterase 5 Inhibitors chemistry, Phosphodiesterase 5 Inhibitors analysis, Phosphodiesterase 5 Inhibitors pharmacology, Magnetic Resonance Spectroscopy methods, Temperature

Abstract

Hydroxycarbodenafil, an analogue of carbodenafil, was detected in a dietary supplement in China in 2020. However, previous reports have not identified some carbon signals from the piperazine ring in nuclear magnetic resonance (NMR) experiments. Because the compound contains an amide bond, the reaction was suggested to be characteristic of compounds with rotational isomers. Variable-temperature NMR is used to determine the rotational barrier between different conformations by changing the measurement temperature. Using this technique, we succeeded in obtaining the first distinct data, including the carbon signals of the piperazine ring in the NMR spectrum of hydroxycarbodenafil. We also confirmed that this technique could be applied to other carbodenafil analogues. Multi-stage mass spectrometry (MS n ) measurements with a high-resolution mass spectrometer specific to the substructures were performed to develop a protocol for the structural determination of the carbodenafil analogues. In addition, hydroxycarbodenafil was analysed using X-ray crystallography, and its inhibitory activity against phosphodiesterase type 5 (PDE5) was measured. The IC 50 value of the inhibitory activity of hydroxycarbodenafil for PDE5A1, a PDE5 isoform, of 2.9 nM was lower than the 4.5 nM for sildenafil, a positive control., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

27. Catalyzed syntheses of novel series of spiro thiazolidinone derivatives with nano Fe 2 O 3 : spectroscopic, X-ray, Hirshfeld surface, DFT, biological and docking evaluations.

Author

Abbass EM, El-Rayyes A, Khalil Ali A, El-Farargy AF, Kozakiewicz-Piekarz A, and Ramadan RM

Subjects

Catalysis, Spiro Compounds chemistry, Spiro Compounds chemical synthesis, Spiro Compounds pharmacology, Crystallography, X-Ray methods, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents chemical synthesis, Density Functional Theory, Microbial Sensitivity Tests, Ferric Compounds chemistry, Hydrogen Bonding, Molecular Docking Simulation, Thiazolidines chemistry, Thiazolidines chemical synthesis, Thiazolidines pharmacology

Abstract

Twelve spiro thiazolidinone compounds (A-L) were synthesized via either conventional thermal or ultrasonication techniques using Fe 2 O 3 nanoparticles. The modification of the traditional procedure by using Fe 2 O 3 nanoparticles led to enhancement of the yield of the desired candidates to 78-93% in approximately half reaction time compared with 58-79% without catalyst. The products were fully characterized using different analytical and spectroscopic techniques. The structure of the two derivatives 4-phenyl-1-thia-4-azaspirodecan-3-one (A) and 4-(p-tolyl)-1-thia-4-azaspirodecan-3-one (B) were also determined using single crystal X-ray diffraction and Hirshfeld surface analysis. The two compounds (A and B) were crystallized in the orthorhombic system with Pbca and P2 1 2 1 2 1 space groups, respectively. In addition, the crystal packing of compounds revealed the formation of supramolecular array with a net of intermolecular hydrogen bonding interactions. The energy optimized geometries of some selected derivatives were performed by density functional theory (DFT/B3LYP). The reactivity descriptors were also calculated and correlated with their biological properties. All the reported compounds were screened for antimicrobial inhibitions. The two derivatives, F and J, exhibited the highest levels of bacterial inhibition with an inhibition zone of 10-17 mm. Also, the two derivatives, F and J, displayed the most potent fungal inhibition with an inhibition zone of 15-23 mm. Molecular docking investigations of some selected derivatives were performed using a B-DNA (PDB: 1BNA) as a macromolecular target. Structure and activity relationship of the reported compounds were correlated with the data of antimicrobial activities and the computed reactivity parameters., (© 2024. The Author(s).)

Published

2024

28. Tale of Two Polymorphs: Investigating the Structural Differences and Dynamic Relationship between Nirmatrelvir Solid Forms (Paxlovid).

Author

Sadeghi MS, Guo R, Bellucci MA, Quino J, Buckle EL, Nisbet ML, Yang Z, Greenwell C, Gorka DE, Pickard Iv FC, Wood GPF, Sun G, Wen SH, Krzyzaniak JF, Meenan PA, Hancock BC, and Yang XH

Subjects

Crystallography, X-Ray methods, Magnetic Resonance Spectroscopy methods, Spectrum Analysis, Raman methods, SARS-CoV-2 drug effects, Transition Temperature, Antiviral Agents chemistry, Crystallization, COVID-19 Drug Treatment, Molecular Dynamics Simulation, X-Ray Diffraction methods

Abstract

Two anhydrous polymorphs of the novel antiviral medicine nirmatrelvir were discovered during the development of Paxlovid, Pfizer's oral Covid-19 treatment. A comprehensive experimental and computational approach was necessary to distinguish the two closely related polymorphs, herein identified as Forms 1 and 4. This approach paired experimental methods, including powder X-ray diffraction and single-crystal X-ray diffraction, solid-state experimental methods, thermal analysis, solid-state nuclear magnetic resonance and Raman spectroscopy with computational investigations comprising crystal structure prediction, Gibbs free energy calculations, and molecular dynamics simulations of the polymorphic transition. Forms 1 and 4 were ultimately determined to be enantiotropically related polymorphs with Form 1 being the stable form above the transition temperature of ∼17 °C and designated as the nominated form for drug development. The work described in this paper shows the importance of using highly specialized orthogonal approaches to elucidate the subtle differences in structure and properties of similar solid-state forms. This synergistic approach allowed for unprecedented speed in bringing Paxlovid to patients in record time amidst the pandemic.

Published

2024

29. Anticancer, antimicrobial and photocatalytic activities of a new pyrazole containing thiosemicarbazone ligand and its Co(III) and Ni(II) complexes: Synthesis, spectroscopic characterization and X-ray crystallography.

Author

Saha M, Mandal S, Sarkar S, Biswas A, Ghati A, Cordes DB, Slawin AMZ, and Saha NC

Subjects

Humans, Crystallography, X-Ray methods, Ligands, Cell Line, Tumor, Catalysis, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents chemical synthesis, Microbial Sensitivity Tests, Thiosemicarbazones chemistry, Nickel chemistry, Cobalt chemistry, Pyrazoles chemistry, Pyrazoles pharmacology, Pyrazoles chemical synthesis, Antineoplastic Agents pharmacology, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Coordination Complexes pharmacology, Coordination Complexes chemical synthesis, Coordination Complexes chemistry

Abstract

A new pyrazole based thiosemicarbazone ligand, 5-methyl-3-formylpyrazole-N(4)-isopropylthiosemicarbazone, (HMP z NHPr i ) (compound I), and its cobalt(III) and nickel(II) complexes, [Co(MP z NHPr i ) 2 ]Cl (compound II) and [Ni(HMP z NHPr i ) 2 ]Br 2 (compound III), respectively, have been synthesized and characterized through various physico-chemical and spectroscopic studies. Both the reported Co(III) and Ni(II) complexes are cationic in nature and behave as 1:1 and 1:2 electrolytes in MeOH, respectively. Electronic spectral features of the complexes have classified them as distorted octahedral ones. IR spectral data (4000-450 cm -1 ) have suggested a monoprotic tridentate (NNS) function of compound I coordinating to the Co(III) ion via the pyrazolyl (tertiary) ring nitrogen, azomethine nitrogen and thiolato sulphur atom; while for compound III, compound I has been found to act as neutral NNS tridentate one, coordinating to Ni(II) via the pyrazolyl iminic nitrogen, azomethine nitrogen and thioketo sulphur. Structural features of all the compounds are confirmed by the single crystal X-ray data. All the compounds reported here have been found to exhibit significant photocatalytic activity towards degradation of Methylene Blue (MB) under UV radiation. Anticancer activity of all the three compounds against cancer cell lines (HeLa and A549) and a normal cell line (HEK293) have been investigated. Compound II has been found to be more efficient against the human cervical cancer cell (HeLa) and the lung cancer cell (A549) than compounds I and III. The ligand and both the complexes display potential activities against both gram-positive (Bacillus subtilis MTCC 7193) and gram-negative bacteria (E. coli MTCC 1610)., Competing Interests: Declaration of competing interest There is no potential conflict of interest to be disclosed., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

30. Preparing research samples for safe arrival at centers and facilities: recipes for successful experiments.

Author

Bowman SEJ, Byrnes J, Russi S, and Zimanyi CM

Subjects

Crystallography, X-Ray methods, Specimen Handling methods, Specimen Handling standards

Abstract

Preparation of biomacromolecules for structural biology studies is a complex and time-consuming process. The goal is to produce a highly concentrated, highly pure product that is often shipped to large facilities with tools to prepare the samples for crystallization trials or for measurements at synchrotrons and cryoEM centers. The aim of this article is to provide guidance and to discuss general considerations for shipping biomacromolecular samples. Details are also provided about shipping samples for specific experiment types, including solution- and cryogenic-based techniques. These guidelines are provided with the hope that the time and energy invested in sample preparation is not lost due to shipping logistics., (open access.)

Published

2024

31. A snapshot love story: what serial crystallography has done and will do for us.

Author

Henkel A and Oberthür D

Subjects

Crystallography, X-Ray methods, Proteins chemistry, Lasers, Models, Molecular, Humans, Synchrotrons

Abstract

Serial crystallography, born from groundbreaking experiments at the Linac Coherent Light Source in 2009, has evolved into a pivotal technique in structural biology. Initially pioneered at X-ray free-electron laser facilities, it has now expanded to synchrotron-radiation facilities globally, with dedicated experimental stations enhancing its accessibility. This review gives an overview of current developments in serial crystallography, emphasizing recent results in time-resolved crystallography, and discussing challenges and shortcomings., (open access.)

Published

2024

32. A first-in-class dimethyl 2-acetamido terephthalate inhibitor targeting Conyza canadensis SHMT1 with a novel herbicidal mode-of-action.

Author

Luo D, Bai Z, Bai H, Liu N, Han J, Ma C, Wu D, Bai L, and Li Z

Subjects

Phthalic Acids pharmacology, Phthalic Acids chemistry, Crystallography, X-Ray methods, Plant Proteins metabolism, Enzyme Inhibitors pharmacology, Enzyme Inhibitors chemistry, Herbicides pharmacology, Herbicides chemistry, Molecular Docking Simulation, Glycine Hydroxymethyltransferase antagonists & inhibitors, Glycine Hydroxymethyltransferase metabolism, Conyza chemistry

Abstract

Introduction: Herbicide application is a highly efficiency method of weed control that boots agricultural output and assures food security. The development of novel herbicides focuses on improved bioactivity and new modes of action. The amino acid biosynthesis was validated as a promising novel mode of action for herbicidal compounds. However, the amino acid biosynthesis enzyme remains largely unexplored for herbicidal targets., Objectives: Serine hydroxymethyl transferase (SHMT) is an essentialenzyme in the photorespiratory cycle. The study aims to explore Conyza canadensis SHMT1 (CcSHMT1) as a promising target for herbicide discovery., Methods: Structure determination of CcSHMT1 was resolved by X-ray crystallography. Virtual screening docking experiments were performed with Glide version 5.5. Novel derivatives of dimethyl 2-acetamido terephthalate were further designed, synthesized, and bioassay. The druggability of the inhibitor was evidenced by ultrastructural changes in mitochondria, in vivo and vitro enzyme activity assays, and genetics analysis., Results: CcSHMT1 has a typical PLP-dependent enzyme 3D structure. The dimethyl 2-acetamido terephthalate-containing compounds had herbicidal activity. Dimethyl 2-(2-(4-(2-(4-bromo-2-chlorophenoxy) acetyl)piperazin-1-yl)acetamido) terephthalate (Compound 9ay, EC 50  = 193.8 g a.i./ ha) exhibited the highest herbicidal activity on tested weed among the synthesized compounds. Compound 9ay had no obvious adverse effect on the growth of maize and honeybees. Compound 9ay was verified to target CcSHMT1 as an herbicide candidate., Conclusion: A first-in-class CcSHMT1 inhibitor that could be developed as a potent herbicide with a new mode of action and provide an avenue for discovering novel inhibitors of pyridoxal-5-phosphate-dependent enzymes., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Production and hosting by Elsevier B.V.)

Published

2024

33. Cryo2RT: a high-throughput method for room-temperature macromolecular crystallography from cryo-cooled crystals.

Author

Huang CY, Aumonier S, Olieric V, and Wang M

Subjects

Crystallography, X-Ray methods, SARS-CoV-2 chemistry, Crystallization methods, Temperature, Models, Molecular, Protein Conformation, Humans, High-Throughput Screening Assays methods, Plant Proteins, Coronavirus 3C Proteases chemistry

Abstract

Advances in structural biology have relied heavily on synchrotron cryo-crystallography and cryogenic electron microscopy to elucidate biological processes and for drug discovery. However, disparities between cryogenic and room-temperature (RT) crystal structures pose challenges. Here, Cryo2RT, a high-throughput RT data-collection method from cryo-cooled crystals that leverages the cryo-crystallography workflow, is introduced. Tested on endothiapepsin crystals with four soaked fragments, thaumatin and SARS-CoV-2 3CL pro , Cryo2RT reveals unique ligand-binding poses, offers a comparable throughput to cryo-crystallography and eases the exploration of structural dynamics at various temperatures., (open access.)

Published

2024

34. Target Identification and Mechanistic Characterization of Indole Terpenoid Mimics: Proper Spindle Microtubule Assembly Is Essential for Cdh1-Mediated Proteolysis of CENP-A.

Author

Peng Y, Zhang Y, Fang R, Jiang H, Lan G, Xu Z, Liu Y, Nie Z, Ren L, Wang F, Zhang SD, Ma Y, Yang P, Ge HH, Zhang WD, Luo C, Li A, and He W

Subjects

Humans, Antigens, CD, Cdh1 Proteins metabolism, Cdh1 Proteins genetics, Crystallography, X-Ray methods, Indoles metabolism, Indoles pharmacology, Indoles chemistry, Spindle Apparatus metabolism, Spindle Apparatus drug effects, Structure-Activity Relationship, Centromere Protein A metabolism, Centromere Protein A genetics, Microtubules metabolism, Microtubules drug effects, Proteolysis drug effects

Abstract

Centromere protein A (CENP-A), a centromere-specific histone H3 variant, is crucial for kinetochore positioning and chromosome segregation. However, its regulatory mechanism in human cells remains incompletely understood. A structure-activity relationship (SAR) study of the cell-cycle-arresting indole terpenoid mimic JP18 leads to the discovery of two more potent analogs, (+)-6-Br-JP18 and (+)-6-Cl-JP18. Tubulin is identified as a potential cellular target of these halogenated analogs by using the drug affinity responsive target stability (DARTS) based method. X-ray crystallography analysis reveals that both molecules bind to the colchicine-binding site of β-tubulin. Treatment of human cells with microtubule-targeting agents (MTAs), including these two compounds, results in CENP-A accumulation by destabilizing Cdh1, a co-activator of the anaphase-promoting complex/cyclosome (APC/C) E3 ubiquitin ligase. This study establishes a link between microtubule dynamics and CENP-A accumulation using small-molecule tools and highlights the role of Cdh1 in CENP-A proteolysis., (© 2024 The Author(s). Advanced Science published by Wiley‐VCH GmbH.)

Published

2024

35. Managing macromolecular crystallographic data with a laboratory information management system.

Author

Daniel E, Wierenga RK, and Lehtiö L

Subjects

Crystallography, X-Ray methods, Proteins chemistry, Software, Databases, Protein, Macromolecular Substances chemistry

Abstract

Protein crystallography is an established method to study the atomic structures of macromolecules and their complexes. A prerequisite for successful structure determination is diffraction-quality crystals, which may require extensive optimization of both the protein and the conditions, and hence projects can stretch over an extended period, with multiple users being involved. The workflow from crystallization and crystal treatment to deposition and publication is well defined, and therefore an electronic laboratory information management system (LIMS) is well suited to management of the data. Completion of the project requires key information on all the steps being available and this information should also be made available according to the FAIR principles. As crystallized samples are typically shipped between facilities, a key feature to be captured in the LIMS is the exchange of metadata between the crystallization facility of the home laboratory and, for example, synchrotron facilities. On completion, structures are deposited in the Protein Data Bank (PDB) and the LIMS can include the PDB code in its database, completing the chain of custody from crystallization to structure deposition and publication. A LIMS designed for macromolecular crystallography, IceBear, is available as a standalone installation and as a hosted service, and the implementation of key features for the capture of metadata in IceBear is discussed as an example., (open access.)

Published

2024

36. Structure Revision of the Fungal Phytotoxin Cavoxin and of Its Corresponding Chroman-4-one Cavoxone by X-ray Crystallography.

Author

Tuzi A, Carbone M, Ciavatta ML, and Evidente A

Subjects

Crystallography, X-Ray methods, Molecular Structure, Ascomycota chemistry, Chromans chemistry, Chromans pharmacology, Mycotoxins chemistry, Mycotoxins pharmacology

Abstract

Cavoxin ( 1 ) was isolated as the main phytotoxin produced by Phoma cava Schulzer, a toxigenic fungus isolated from Castanea spp. Its structure was determined by 1D NMR and MS in 1985 along with that of the corresponding chroman-4-one cavoxone ( 2 ), an artifact formed by acid treatment of 1 . Since that time cavoxin was shown to be phytotoxic, antifungal, antifeedant, herbicidal, and antirust with potential application in agriculture and medicine. During a study aimed at improving cavoxin's production by P. cava , single crystals for X-ray diffractometric analysis were obtained. The X-ray crystallography characterization confirmed only in part the structure proposed for cavoxin ( 1 ), revealing a different substitution pattern on the aromatic ring, as depicted in the revised structure 3 .

Published

2024

37. Bridging the microscopic divide: a comprehensive overview of micro-crystallization and in vivo crystallography.

Author

Chavas LMG, Coulibaly F, and Garriga D

Subjects

Crystallography, X-Ray methods, Crystallography methods, Macromolecular Substances chemistry, Crystallization

Abstract

A series of events underscoring the significant advancements in micro-crystallization and in vivo crystallography were held during the 26th IUCr Congress in Melbourne, positioning microcrystallography as a pivotal field within structural biology. Through collaborative discussions and the sharing of innovative methodologies, these sessions outlined frontier approaches in macromolecular crystallography. This review provides an overview of this rapidly moving field in light of the rich dialogues and forward-thinking proposals explored during the congress workshop and microsymposium. These advances in microcrystallography shed light on the potential to reshape current research paradigms and enhance our comprehension of biological mechanisms at the molecular scale., (open access.)

Published

2024

38. Deep-learning map segmentation for protein X-ray crystallographic structure determination.

Author

Skubák P

Subjects

Crystallography, X-Ray methods, Protein Conformation, Neural Networks, Computer, Databases, Protein, Models, Molecular, Deep Learning, Proteins chemistry

Abstract

When solving a structure of a protein from single-wavelength anomalous diffraction X-ray data, the initial phases obtained by phasing from an anomalously scattering substructure usually need to be improved by an iterated electron-density modification. In this manuscript, the use of convolutional neural networks (CNNs) for segmentation of the initial experimental phasing electron-density maps is proposed. The results reported demonstrate that a CNN with U-net architecture, trained on several thousands of electron-density maps generated mainly using X-ray data from the Protein Data Bank in a supervised learning, can improve current density-modification methods., (open access.)

Published

2024

39. A structural role for tryptophan in proteins, and the ubiquitous Trp C δ1 -H...O=C (backbone) hydrogen bond.

Author

Szczygiel M, Derewenda U, Scheiner S, Minor W, and Derewenda ZS

Subjects

Models, Molecular, Crystallography, X-Ray methods, Protein Conformation, Tryptophan chemistry, Hydrogen Bonding, Proteins chemistry

Abstract

Tryptophan is the most prominent amino acid found in proteins, with multiple functional roles. Its side chain is made up of the hydrophobic indole moiety, with two groups that act as donors in hydrogen bonds: the N ϵ -H group, which is a potent donor in canonical hydrogen bonds, and a polarized C δ1 -H group, which is capable of forming weaker, noncanonical hydrogen bonds. Due to adjacent electron-withdrawing moieties, C-H...O hydrogen bonds are ubiquitous in macromolecules, albeit contingent on the polarization of the donor C-H group. Consequently, C α -H groups (adjacent to the carbonyl and amino groups of flanking peptide bonds), as well as the C ϵ1 -H and C δ2 -H groups of histidines (adjacent to imidazole N atoms), are known to serve as donors in hydrogen bonds, for example stabilizing parallel and antiparallel β-sheets. However, the nature and the functional role of interactions involving the C δ1 -H group of the indole ring of tryptophan are not well characterized. Here, data mining of high-resolution (r ≤ 1.5 Å) crystal structures from the Protein Data Bank was performed and ubiquitous close contacts between the C δ1 -H groups of tryptophan and a range of electronegative acceptors were identified, specifically main-chain carbonyl O atoms immediately upstream and downstream in the polypeptide chain. The stereochemical analysis shows that most of the interactions bear all of the hallmarks of proper hydrogen bonds. At the same time, their cohesive nature is confirmed by quantum-chemical calculations, which reveal interaction energies of 1.5-3.0 kcal mol -1 , depending on the specific stereochemistry., (open access.)

Published

2024

40. Towards a dependable data set of structures for L-asparaginase research.

Author

Wlodawer A, Dauter Z, Lubkowski J, Loch JI, Brzezinski D, Gilski M, and Jaskolski M

Subjects

Humans, Models, Molecular, Crystallography, X-Ray methods, Protein Conformation, Asparaginase chemistry, Databases, Protein

Abstract

The Protein Data Bank (PDB) includes a carefully curated treasury of experimentally derived structural data on biological macromolecules and their various complexes. Such information is fundamental for a multitude of projects that involve large-scale data mining and/or detailed evaluation of individual structures of importance to chemistry, biology and, most of all, to medicine, where it provides the foundation for structure-based drug discovery. However, despite extensive validation mechanisms, it is almost inevitable that among the ∼215 000 entries there will occasionally be suboptimal or incorrect structure models. It is thus vital to apply careful verification procedures to those segments of the PDB that are of direct medicinal interest. Here, such an analysis was carried out for crystallographic models of L-asparaginases, enzymes that include approved drugs for the treatment of certain types of leukemia. The focus was on the adherence of the atomic coordinates to the rules of stereochemistry and their agreement with the experimental electron-density maps. Whereas the current clinical application of L-asparaginases is limited to two bacterial proteins and their chemical modifications, the field of investigations of such enzymes has expanded tremendously in recent years with the discovery of three entirely different structural classes and with numerous reports, not always quite reliable, of the anticancer properties of L-asparaginases of different origins.

Published

2024

41. Automated multiconformer model building for X-ray crystallography and cryo-EM.

Author

Wankowicz SA, Ravikumar A, Sharma S, Riley B, Raju A, Hogan DW, Flowers J, van den Bedem H, Keedy DA, and Fraser JS

Subjects

Crystallography, X-Ray methods, Proteins chemistry, Software, Algorithms, Computational Biology methods, Cryoelectron Microscopy methods, Models, Molecular, Protein Conformation

Abstract

In their folded state, biomolecules exchange between multiple conformational states that are crucial for their function. Traditional structural biology methods, such as X-ray crystallography and cryogenic electron microscopy (cryo-EM), produce density maps that are ensemble averages, reflecting molecules in various conformations. Yet, most models derived from these maps explicitly represent only a single conformation, overlooking the complexity of biomolecular structures. To accurately reflect the diversity of biomolecular forms, there is a pressing need to shift toward modeling structural ensembles that mirror the experimental data. However, the challenge of distinguishing signal from noise complicates manual efforts to create these models. In response, we introduce the latest enhancements to qFit, an automated computational strategy designed to incorporate protein conformational heterogeneity into models built into density maps. These algorithmic improvements in qFit are substantiated by superior R free and geometry metrics across a wide range of proteins. Importantly, unlike more complex multicopy ensemble models, the multiconformer models produced by qFit can be manually modified in most major model building software (e.g., Coot) and fit can be further improved by refinement using standard pipelines (e.g., Phenix, Refmac, Buster). By reducing the barrier of creating multiconformer models, qFit can foster the development of new hypotheses about the relationship between macromolecular conformational dynamics and function., Competing Interests: SW, AR, SS, BR, AR, DH, JF, DK, JF No competing interests declared, Hv The work in this publication does not overlap with Henry van den Bedem's role at Atomwise Inc, and there is no conflict of interest, (© 2023, Wankowicz et al.)

Published

2024

42. Protein purification, crystallization, and structure determination of transcription factor YhaJ in complex with DNT metabolites.

Author

Kim M, Kang R, Jeon TJ, and Ryu SE

Subjects

Dinitrobenzenes chemistry, Crystallography, X-Ray methods, Transcription Factors metabolism, Transcription Factors chemistry, Transcription Factors isolation & purification, Bacterial Proteins chemistry, Bacterial Proteins isolation & purification, Bacterial Proteins metabolism, Crystallization

Abstract

The microbial transcription factor YhaJ responds to 2,4-dinitrotoluene (DNT) derivatives. Here, we describe steps for overexpression and purification of the protein, characterization for the binding of a DNT derivative methylhydroquinone, and crystallization by using a random seeding technique. We then detail procedures for structure determination by employing the crystal-twin resolving processes. This protocol can also be performed using other DNT derivatives. For complete details on the use and execution of this protocol, please refer to Kim et al. 1 ., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

43. High-throughput structure determination of an intrinsically disordered protein using cell-free protein crystallization.

Author

Kojima M, Abe S, Furuta T, Hirata K, Yao X, Kobayashi A, Kobayashi R, and Ueno T

Subjects

Crystallography, X-Ray methods, Humans, Protein Conformation, Models, Molecular, Protein Binding, Intrinsically Disordered Proteins chemistry, Crystallization, Proto-Oncogene Proteins c-myc chemistry, Proto-Oncogene Proteins c-myc genetics, Proto-Oncogene Proteins c-myc metabolism, Cell-Free System

Abstract

Intrinsically disordered proteins (IDPs) play a crucial role in various biological phenomena, dynamically changing their conformations in response to external environmental cues. To gain a deeper understanding of these proteins, it is essential to identify the determinants that fix their structures at the atomic level. Here, we developed a pipeline for rapid crystal structure analysis of IDP using a cell-free protein crystallization (CFPC) method. Through this approach, we successfully demonstrated the determination of the structure of an IDP to uncover the key determinants that stabilize its conformation. Specifically, we focused on the 11-residue fragment of c-Myc, which forms an α-helix through dimerization with a binding partner protein. This fragment was strategically recombined with an in-cell crystallizing protein and was expressed in a cell-free system. The resulting crystal structures of the c-Myc fragment were successfully determined at a resolution of 1.92 Å and we confirmed that they are identical to the structures of the complex with the native binding partner protein. This indicates that the environment of the scaffold crystal can fix the structure of c-Myc. Significantly, these crystals were obtained directly from a small reaction mixture (30 µL) incubated for only 72 h. Analysis of eight crystal structures derived from 22 mutants revealed two hydrophobic residues as the key determinants responsible for stabilizing the α-helical structure. These findings underscore the power of our CFPC screening method as a valuable tool for determining the structures of challenging target proteins and elucidating the essential molecular interactions that govern their stability., Competing Interests: Competing interests statement:The authors declare no competing interest.

Published

2024

44. Biological Activity of Complexes Involving Nitro-Containing Ligands and Crystallographic-Theoretical Description of 3,5-DNB Complexes.

Author

Fonseca-López D, Lozano JD, Macías MA, Muñoz-Castro Á, MacLeod-Carey D, Nagles E, and Hurtado J

Subjects

Ligands, Nitrobenzoates chemistry, Nitrobenzoates pharmacology, Humans, Crystallography, X-Ray methods, Nitro Compounds chemistry, Nitro Compounds pharmacology, Coordination Complexes chemistry, Coordination Complexes pharmacology

Abstract

Drug resistance in infectious diseases developed by bacteria and fungi is an important issue since it is necessary to further develop novel compounds with biological activity that counteract this problem. In addition, new pharmaceutical compounds with lower secondary effects to treat cancer are needed. Coordination compounds appear to be accessible and promising alternatives aiming to overcome these problems. In this review, we summarize the recent literature on coordination compounds based on nitrobenzoic acid (NBA) as a ligand, its derivatives, and other nitro-containing ligands, which are widely employed owing to their versatility. Additionally, an analysis of crystallographic data is presented, unraveling the coordination preferences and the most effective crystallization methods to grow crystals of good quality. This underscores the significance of elucidating crystalline structures and utilizing computational calculations to deepen the comprehension of the electronic properties of coordination complexes., Competing Interests: The authors declare no conflict of interest.

Published

2024

45. Room-temperature serial synchrotron crystallography structure of Spinacia oleracea RuBisCO.

Author

Bjelčić M, Aurelius O, Nan J, Neutze R, and Ursby T

Subjects

Crystallography, X-Ray methods, Temperature, Protein Conformation, Spinacia oleracea enzymology, Spinacia oleracea chemistry, Ribulose-Bisphosphate Carboxylase chemistry, Ribulose-Bisphosphate Carboxylase metabolism, Synchrotrons, Models, Molecular

Abstract

Ribulose-1,5-bisphosphate carboxylase/oxygenase (RuBisCO) is the enzyme responsible for the first step of carbon dioxide (CO 2 ) fixation in plants, which proceeds via the carboxylation of ribulose 1,5-biphosphate. Because of the enormous importance of this reaction in agriculture and the environment, there is considerable interest in the mechanism of fixation of CO 2 by RuBisCO. Here, a serial synchrotron crystallography structure of spinach RuBisCO is reported at 2.3 Å resolution. This structure is consistent with earlier single-crystal X-ray structures of this enzyme and the results are a good starting point for a further push towards time-resolved serial synchrotron crystallography in order to better understand the mechanism of the reaction., (open access.)

Published

2024

46. High-confidence placement of low-occupancy fragments into electron density using the anomalous signal of sulfur and halogen atoms.

Author

Ma S, Damfo S, Bowler MW, Mykhaylyk V, and Kozielski F

Subjects

Crystallography, X-Ray methods, Viral Nonstructural Proteins chemistry, Humans, Electrons, Models, Molecular, Drug Design, Protein Binding, Binding Sites, COVID-19, Halogens chemistry, Sulfur chemistry, SARS-CoV-2 chemistry

Abstract

Fragment-based drug design using X-ray crystallography is a powerful technique to enable the development of new lead compounds, or probe molecules, against biological targets. This study addresses the need to determine fragment binding orientations for low-occupancy fragments with incomplete electron density, an essential step before further development of the molecule. Halogen atoms play multiple roles in drug discovery due to their unique combination of electronegativity, steric effects and hydrophobic properties. Fragments incorporating halogen atoms serve as promising starting points in hit-to-lead development as they often establish halogen bonds with target proteins, potentially enhancing binding affinity and selectivity, as well as counteracting drug resistance. Here, the aim was to unambiguously identify the binding orientations of fragment hits for SARS-CoV-2 nonstructural protein 1 (nsp1) which contain a combination of sulfur and/or chlorine, bromine and iodine substituents. The binding orientations of carefully selected nsp1 analogue hits were focused on by employing their anomalous scattering combined with Pan-Dataset Density Analysis (PanDDA). Anomalous difference Fourier maps derived from the diffraction data collected at both standard and long-wavelength X-rays were compared. The discrepancies observed in the maps of iodine-containing fragments collected at different energies were attributed to site-specific radiation-damage stemming from the strong X-ray absorption of I atoms, which is likely to cause cleavage of the C-I bond. A reliable and effective data-collection strategy to unambiguously determine the binding orientations of low-occupancy fragments containing sulfur and/or halogen atoms while mitigating radiation damage is presented., (open access.)

Published

2024

47. Unveiling success determinants for AMB-assisted phase expansion of fusion proteins in ARP/wARP.

Author

Cardona-Echavarría MC, Santillán C, Miranda-Blancas R, Stojanoff V, and Rudiño-Piñera E

Subjects

Crystallography, X-Ray methods, Glutathione Transferase genetics, Glutathione Transferase chemistry, Glutathione Transferase metabolism, Thioredoxins chemistry, Thioredoxins genetics, Thioredoxins metabolism, Models, Molecular, Databases, Protein, Crystallization methods, Protein Conformation, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins metabolism, Green Fluorescent Proteins metabolism, Green Fluorescent Proteins genetics, Green Fluorescent Proteins chemistry, Maltose-Binding Proteins genetics, Maltose-Binding Proteins chemistry, Maltose-Binding Proteins metabolism

Abstract

Fusion proteins (FPs) are frequently utilized as a biotechnological tool in the determination of macromolecular structures using X-ray methods. Here, we explore the use of different protein tags in various FP, to obtain initial phases by using them in a partial molecular replacement (MR) and constructing the remaining FP structure with ARP/wARP. Usually, the tag is removed prior to crystallization, however leaving the tag on may facilitate crystal formation, and structural determination by expanding phases from known to unknown segments of the complex. In this study, the Protein Data Bank was mined for an up-to-date list of FPs with the most used protein tags, Maltose Binding Protein (MBP), Green Fluorescent Protein (GFP), Thioredoxin (TRX), Glutathione transferase (GST) and the Small Ubiquitin-like Modifier Protein (SUMO). Partial MR using the protein tag, followed by automatic model building, was tested on a subset of 116 FP. The efficiency of this method was analyzed and factors that influence the coordinate construction of a substantial portions of the fused protein were identified. Using MBP, GFP, and SUMO as phase generators it was possible to build at least 75 % of the protein of interest in 36 of the 116 cases tested. Our results reveal that tag selection has a significant impact; tags with greater structural stability, such as GFP, increase the success rate. Further statistical analysis identifies that resolution, Wilson B factor, solvent percentage, completeness, multiplicity, protein tag percentage in the FP (considering amino acids), and the linker length play pivotal roles using our approach. In cases where a structural homologous is absent, this method merits inclusion in the toolkit of protein crystallographers., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

48. An alternative conformation of the N-terminal loop of human dihydroorotate dehydrogenase drives binding to a potent antiproliferative agent.

Author

Alberti M, Poli G, Broggini L, Sainas S, Rizzi M, Boschi D, Ferraris DM, Martino E, Ricagno S, Tuccinardi T, Lolli ML, and Miggiano R

Subjects

Humans, Crystallography, X-Ray methods, Binding Sites, Pyridines chemistry, Pyridines pharmacology, Protein Conformation, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Models, Molecular, Protein Binding, Hydrogen Bonding, Dihydroorotate Dehydrogenase, Oxidoreductases Acting on CH-CH Group Donors chemistry, Oxidoreductases Acting on CH-CH Group Donors antagonists & inhibitors, Oxidoreductases Acting on CH-CH Group Donors metabolism

Abstract

Over the years, human dihydroorotate dehydrogenase (hDHODH), which is a key player in the de novo pyrimidine-biosynthesis pathway, has been targeted in the treatment of several conditions, including autoimmune disorders and acute myelogenous leukaemia, as well as in host-targeted antiviral therapy. A molecular exploration of its inhibitor-binding behaviours yielded promising candidates for innovative drug design. A detailed description of the enzymatic pharmacophore drove the decoration of well-established inhibitory scaffolds, thus gaining further in vitro and in vivo efficacy. In the present work, using X-ray crystallography, an atypical rearrangement was identified in the binding pose of a potent inhibitor characterized by a polar pyridine-based moiety (compound 18). The crystal structure shows that upon binding compound 18 the dynamics of a protein loop involved in a gating mechanism at the cofactor-binding site is modulated by the presence of three water molecules, thus fine-tuning the polarity/hydrophobicity of the binding pocket. These solvent molecules are engaged in the formation of a hydrogen-bond mesh in which one of them establishes a direct contact with the pyridine moiety of compound 18, thus paving the way for a reappraisal of the inhibition of hDHODH. Using an integrated approach, the thermodynamics of such a modulation is described by means of isothermal titration calorimetry coupled with molecular modelling. These structural insights will guide future drug design to obtain a finer K d /logD 7.4 balance and identify membrane-permeable molecules with a drug-like profile in terms of water solubility.

Published

2024

49. Ultrapotent influenza hemagglutinin fusion inhibitors developed through SuFEx-enabled high-throughput medicinal chemistry.

Author

Kitamura S, Lin TH, Lee CD, Takamura A, Kadam RU, Zhang D, Zhu X, Dada L, Nagai E, Yu W, Yao Y, Sharpless KB, Wilson IA, and Wolan DW

Subjects

Humans, Chemistry, Pharmaceutical methods, High-Throughput Screening Assays methods, Influenza, Human drug therapy, Influenza, Human virology, Crystallography, X-Ray methods, Click Chemistry methods, Animals, Influenza A virus drug effects, Madin Darby Canine Kidney Cells, Viral Fusion Protein Inhibitors pharmacology, Viral Fusion Protein Inhibitors chemistry, Dogs, Hemagglutinin Glycoproteins, Influenza Virus metabolism, Hemagglutinin Glycoproteins, Influenza Virus chemistry, Antiviral Agents pharmacology, Antiviral Agents chemistry

Abstract

Seasonal and pandemic-associated influenza strains cause highly contagious viral respiratory infections that can lead to severe illness and excess mortality. Here, we report on the optimization of our small-molecule inhibitor F0045(S) targeting the influenza hemagglutinin (HA) stem with our Sulfur-Fluoride Exchange (SuFEx) click chemistry-based high-throughput medicinal chemistry (HTMC) strategy. A combination of SuFEx- and amide-based lead molecule diversification and structure-guided design led to identification and validation of ultrapotent influenza fusion inhibitors with subnanomolar EC 50 cellular antiviral activity against several influenza A group 1 strains. X-ray structures of six of these compounds with HA indicate that the appended moieties occupy additional pockets on the HA surface and increase the binding interaction, where the accumulation of several polar interactions also contributes to the improved affinity. The compounds here represent the most potent HA small-molecule inhibitors to date. Our divergent HTMC platform is therefore a powerful, rapid, and cost-effective approach to develop bioactive chemical probes and drug-like candidates against viral targets., Competing Interests: Competing interests statement:The authors declare no competing interest.

Published

2024

50. Emerging Topics in Protein Crystallography.

Author

Chen Z and Zanotti G

Subjects

Crystallography, X-Ray methods, Protein Conformation, Humans, Proteins chemistry

Abstract

Protein crystallography is the discipline concerned with the determination of the three-dimensional structure of biological macromolecules in a crystalline state [...].

Published

2024