Your search keyword '"Armin Wagner"' showing total 220 results

1. Molecular mechanism of BMP signal control by Twisted gastrulation

Author

Tomas Malinauskas, Gareth Moore, Amalie F. Rudolf, Holly Eggington, Hayley L. Belnoue-Davis, Kamel El Omari, Samuel C. Griffiths, Rachel E. Woolley, Ramona Duman, Armin Wagner, Simon J. Leedham, Clair Baldock, Hilary L. Ashe, and Christian Siebold

Subjects

Science

Abstract

Abstract Twisted gastrulation (TWSG1) is an evolutionarily conserved secreted glycoprotein which controls signaling by Bone Morphogenetic Proteins (BMPs). TWSG1 binds BMPs and their antagonist Chordin to control BMP signaling during embryonic development, kidney regeneration and cancer. We report crystal structures of TWSG1 alone and in complex with a BMP ligand, Growth Differentiation Factor 5. TWSG1 is composed of two distinct, disulfide-rich domains. The TWSG1 N-terminal domain occupies the BMP type 1 receptor binding site on BMPs, whereas the C-terminal domain binds to a Chordin family member. We show that TWSG1 inhibits BMP function in cellular signaling assays and mouse colon organoids. This inhibitory function is abolished in a TWSG1 mutant that cannot bind BMPs. The same mutation in the Drosophila TWSG1 ortholog Tsg fails to mediate BMP gradient formation required for dorsal-ventral axis patterning of the early embryo. Our studies reveal the evolutionarily conserved mechanism of BMP signaling inhibition by TWSG1.

Published

2024

2. Structure and function of Semaphorin-5A glycosaminoglycan interactions

Author

Gergely N. Nagy, Xiao-Feng Zhao, Richard Karlsson, Karen Wang, Ramona Duman, Karl Harlos, Kamel El Omari, Armin Wagner, Henrik Clausen, Rebecca L. Miller, Roman J. Giger, and E. Yvonne Jones

Subjects

Science

Abstract

Abstract Integration of extracellular signals by neurons is pivotal for brain development, plasticity, and repair. Axon guidance relies on receptor-ligand interactions crosstalking with extracellular matrix components. Semaphorin-5A (Sema5A) is a bifunctional guidance cue exerting attractive and inhibitory effects on neuronal growth through the interaction with heparan sulfate (HS) and chondroitin sulfate (CS) glycosaminoglycans (GAGs), respectively. Sema5A harbors seven thrombospondin type-1 repeats (TSR1-7) important for GAG binding, however the underlying molecular basis and functions in vivo remain enigmatic. Here we dissect the structural basis for Sema5A:GAG specificity and demonstrate the functional significance of this interaction in vivo. Using x-ray crystallography, we reveal a dimeric fold variation for TSR4 that accommodates GAG interactions. TSR4 co-crystal structures identify binding residues validated by site-directed mutagenesis. In vitro and cell-based assays uncover specific GAG epitopes necessary for TSR association. We demonstrate that HS-GAG binding is preferred over CS-GAG and mediates Sema5A oligomerization. In vivo, Sema5A:GAG interactions are necessary for Sema5A function and regulate Plexin-A2 dependent dentate progenitor cell migration. Our study rationalizes Sema5A associated developmental and neurological disorders and provides mechanistic insights into how multifaceted guidance functions of a single transmembrane cue are regulated by proteoglycans.

Published

2024

3. Structure and function of the ROR2 cysteine-rich domain in vertebrate noncanonical WNT5A signaling

Author

Samuel C Griffiths, Jia Tan, Armin Wagner, Levi L Blazer, Jarrett J Adams, Srisathya Srinivasan, Shayan Moghisaei, Sachdev S Sidhu, Christian Siebold, and Hsin-Yi Henry Ho

Subjects

WNT5A, ROR2, Frizzled, cysteine-rich domain, Kringle domain, receptor tyrosine kinase, Medicine, Science, Biology (General), QH301-705.5

Abstract

The receptor tyrosine kinase ROR2 mediates noncanonical WNT5A signaling to orchestrate tissue morphogenetic processes, and dysfunction of the pathway causes Robinow syndrome, brachydactyly B, and metastatic diseases. The domain(s) and mechanisms required for ROR2 function, however, remain unclear. We solved the crystal structure of the extracellular cysteine-rich (CRD) and Kringle (Kr) domains of ROR2 and found that, unlike other CRDs, the ROR2 CRD lacks the signature hydrophobic pocket that binds lipids/lipid-modified proteins, such as WNTs, suggesting a novel mechanism of ligand reception. Functionally, we showed that the ROR2 CRD, but not other domains, is required and minimally sufficient to promote WNT5A signaling, and Robinow mutations in the CRD and the adjacent Kr impair ROR2 secretion and function. Moreover, using function-activating and -perturbing antibodies against the Frizzled (FZ) family of WNT receptors, we demonstrate the involvement of FZ in WNT5A-ROR signaling. Thus, ROR2 acts via its CRD to potentiate the function of a receptor super-complex that includes FZ to transduce WNT5A signals.

Published

2024

4. Experimental phasing opportunities for macromolecular crystallography at very long wavelengths

Author

Kamel El Omari, Ramona Duman, Vitaliy Mykhaylyk, Christian M. Orr, Merlyn Latimer-Smith, Graeme Winter, Vinay Grama, Feng Qu, Kiran Bountra, Hok Sau Kwong, Maria Romano, Rosana I. Reis, Lutz Vogeley, Luca Vecchia, C. David Owen, Sina Wittmann, Max Renner, Miki Senda, Naohiro Matsugaki, Yoshiaki Kawano, Thomas A. Bowden, Isabel Moraes, Jonathan M. Grimes, Erika J. Mancini, Martin A. Walsh, Cristiane R. Guzzo, Raymond J. Owens, E. Yvonne Jones, David G. Brown, Dave I. Stuart, Konstantinos Beis, and Armin Wagner

Subjects

Chemistry, QD1-999

Abstract

Abstract Despite recent advances in cryo-electron microscopy and artificial intelligence-based model predictions, a significant fraction of structure determinations by macromolecular crystallography still requires experimental phasing, usually by means of single-wavelength anomalous diffraction (SAD) techniques. Most synchrotron beamlines provide highly brilliant beams of X-rays of between 0.7 and 2 Å wavelength. Use of longer wavelengths to access the absorption edges of biologically important lighter atoms such as calcium, potassium, chlorine, sulfur and phosphorus for native-SAD phasing is attractive but technically highly challenging. The long-wavelength beamline I23 at Diamond Light Source overcomes these limitations and extends the accessible wavelength range to λ = 5.9 Å. Here we report 22 macromolecular structures solved in this extended wavelength range, using anomalous scattering from a range of elements which demonstrate the routine feasibility of lighter atom phasing. We suggest that, in light of its advantages, long-wavelength crystallography is a compelling option for experimental phasing.

Published

2023

5. Light activation of Orange Carotenoid Protein reveals bicycle-pedal single-bond isomerization

Author

Volha U. Chukhutsina, James M. Baxter, Alisia Fadini, Rhodri M. Morgan, Matthew A. Pope, Karim Maghlaoui, Christian M. Orr, Armin Wagner, and Jasper J. van Thor

Subjects

Science

Abstract

Orange Carotenoid protein (OCP) is the only photoreceptor with a carotenoid for sensing. Here, the authors report crystal structures of the early OCP photoproduct, suggesting that photo-sensing involves single bond isomerization.

Published

2022

6. Structural basis for proton coupled cystine transport by cystinosin

Author

Mark Löbel, Sacha P. Salphati, Kamel El Omari, Armin Wagner, Stephen J. Tucker, Joanne L. Parker, and Simon Newstead

Subjects

Science

Abstract

Mutations in CTNS, the lysosomal cystine-proton symporter, cause cystinosis. Here authors report crystal structures of CTNS from Arabidopsis thaliana in complex with cystine, and establish the mode of ligand recognition and mechanism for proton-coupled cystine export from the lysosome.

Published

2022

7. Structure and assembly of the S-layer in C. difficile

Author

Paola Lanzoni-Mangutchi, Oishik Banerji, Jason Wilson, Anna Barwinska-Sendra, Joseph A. Kirk, Filipa Vaz, Shauna O’Beirne, Arnaud Baslé, Kamel El Omari, Armin Wagner, Neil F. Fairweather, Gillian R. Douce, Per A. Bullough, Robert P. Fagan, and Paula S. Salgado

Subjects

Science

Abstract

The S-layer is a two-dimensional protein array that covers the cell surface of many bacteria and archaea. Here, the authors use high-resolution X-ray crystallography and electron microscopy to provide detailed insights into S-layer organisation and assembly for the bacterial pathogen Clostridioides difficile.

Published

2022

8. Fixed-target serial femtosecond crystallography using in cellulo grown microcrystals

Author

J. Mia Lahey-Rudolph, Robert Schönherr, Miriam Barthelmess, Pontus Fischer, Carolin Seuring, Armin Wagner, Alke Meents, and Lars Redecke

Subjects

fixed-target sfx, serial femtosecond crystallography, in cellulo crystallography, intracellular protein crystals, silicon chip, roadrunner, Crystallography, QD901-999

Abstract

The crystallization of recombinant proteins in living cells is an exciting new approach in structural biology. Recent success has highlighted the need for fast and efficient diffraction data collection, optimally directly exposing intact crystal-containing cells to the X-ray beam, thus protecting the in cellulo crystals from environmental challenges. Serial femtosecond crystallography (SFX) at free-electron lasers (XFELs) allows the collection of detectable diffraction even from tiny protein crystals, but requires very fast sample exchange to utilize each XFEL pulse. Here, an efficient approach is presented for high-resolution structure elucidation using serial femtosecond in cellulo diffraction of micometre-sized crystals of the protein HEX-1 from the fungus Neurospora crassa on a fixed target. Employing the fast and highly accurate Roadrunner II translation-stage system allowed efficient raster scanning of the pores of micro-patterned, single-crystalline silicon chips loaded with living, crystal-containing insect cells. Compared with liquid-jet and LCP injection systems, the increased hit rates of up to 30% and reduced background scattering enabled elucidation of the HEX-1 structure. Using diffraction data from only a single chip collected within 12 min at the Linac Coherent Light Source, a 1.8 Å resolution structure was obtained with significantly reduced sample consumption compared with previous SFX experiments using liquid-jet injection. This HEX-1 structure is almost superimposable with that previously determined using synchrotron radiation from single HEX-1 crystals grown by sitting-drop vapour diffusion, validating the approach. This study demonstrates that fixed-target SFX using micro-patterned silicon chips is ideally suited for efficient in cellulo diffraction data collection using living, crystal-containing cells, and offers huge potential for the straightforward structure elucidation of proteins that form intracellular crystals at both XFELs and synchrotron sources.

Published

2021

9. Experimental phasing with vanadium and application to nucleotide-binding membrane proteins

Author

Kamel El Omari, Nada Mohamad, Kiran Bountra, Ramona Duman, Maria Romano, Katja Schlegel, Hok-Sau Kwong, Vitaliy Mykhaylyk, Claus Olesen, Jesper Vuust Moller, Maike Bublitz, Konstantinos Beis, and Armin Wagner

Subjects

experimental phasing, vanadium, membrane proteins, Crystallography, QD901-999

Abstract

The structure determination of soluble and membrane proteins can be hindered by the crystallographic phase problem, especially in the absence of a suitable homologous structure. Experimental phasing is the method of choice for novel structures; however, it often requires heavy-atom derivatization, which can be difficult and time-consuming. Here, a novel and rapid method to obtain experimental phases for protein structure determination by vanadium phasing is reported. Vanadate is a transition-state mimic of phosphoryl-transfer reactions and it has the advantage of binding specifically to the active site of numerous enzymes catalyzing this reaction. The applicability of vanadium phasing has been validated by determining the structures of three different protein–vanadium complexes, two of which are integral membrane proteins: the rabbit sarcoplasmic reticulum Ca2+-ATPase, the antibacterial peptide ATP-binding cassette transporter McjD from Escherichia coli and the soluble enzyme RNAse A from Bos taurus. Vanadium phasing was successful even at low resolution and despite severe anisotropy in the data. This method is principally applicable to a large number of proteins, representing six of the seven Enzyme Commission classes. It relies exclusively on the specific chemistry of the protein and it does not require any modifications, making it a very powerful addition to the phasing toolkit. In addition to the phasing power of this technique, the protein–vanadium complexes also provide detailed insights into the reaction mechanisms of the studied proteins.

Published

2020

10. Importance of potassium ions for ribosome structure and function revealed by long-wavelength X-ray diffraction

Author

Alexey Rozov, Iskander Khusainov, Kamel El Omari, Ramona Duman, Vitaliy Mykhaylyk, Marat Yusupov, Eric Westhof, Armin Wagner, and Gulnara Yusupova

Subjects

Science

Abstract

Metal ions play essential roles in myriads of biological processes, from catalytic co-factors to supporting protein and nucleic acid structures. Here the authors use long-wavelength X-ray diffraction to locate hundreds of potassium ions taking part in the formation of rRNA tertiary structure, mediating rRNA–protein interactions and supporting ribosomal protein structures and function.

Published

2019

11. The architecture of EMC reveals a path for membrane protein insertion

Author

John P O'Donnell, Ben P Phillips, Yuichi Yagita, Szymon Juszkiewicz, Armin Wagner, Duccio Malinverni, Robert J Keenan, Elizabeth A Miller, and Ramanujan S Hegde

Subjects

endoplasmic reticulum, membrane proteins, organelle biogenesis, chaperone, Medicine, Science, Biology (General), QH301-705.5

Abstract

Approximately 25% of eukaryotic genes code for integral membrane proteins that are assembled at the endoplasmic reticulum. An abundant and widely conserved multi-protein complex termed EMC has been implicated in membrane protein biogenesis, but its mechanism of action is poorly understood. Here, we define the composition and architecture of human EMC using biochemical assays, crystallography of individual subunits, site-specific photocrosslinking, and cryo-EM reconstruction. Our results suggest that EMC’s cytosolic domain contains a large, moderately hydrophobic vestibule that can bind a substrate’s transmembrane domain (TMD). The cytosolic vestibule leads into a lumenally-sealed, lipid-exposed intramembrane groove large enough to accommodate a single substrate TMD. A gap between the cytosolic vestibule and intramembrane groove provides a potential path for substrate egress from EMC. These findings suggest how EMC facilitates energy-independent membrane insertion of TMDs, explain why only short lumenal domains are translocated by EMC, and constrain models of EMC’s proposed chaperone function.

Published

2020

12. Anomalous X-ray diffraction studies of ion transport in K+ channels

Author

Patricia S. Langan, Venu Gopal Vandavasi, Kevin L. Weiss, Pavel V. Afonine, Kamel el Omari, Ramona Duman, Armin Wagner, and Leighton Coates

Subjects

Science

Abstract

The number of K+ occupied binding sites in the selectivity filter of potassium ion channels is still under debate. Here, the authors collect diffraction data on the K+ selective NaK channel NaK2K at a wavelength of 3.35 Å, close to the K absorption edge, revealing that all four binding sites in the selectivity filter are fully occupied by K+ ions.

Published

2018

13. Multimodal Non-Contact Luminescence Thermometry with Cr-Doped Oxides

Author

Vitaliy Mykhaylyk, Hans Kraus, Yaroslav Zhydachevskyy, Volodymyr Tsiumra, Andriy Luchechko, Armin Wagner, and Andrzej Suchocki

Subjects

non-contact luminescence thermometry, luminescence decay thermometry, intensity ratio thermometry, wavelength shift thermometry, Cr3+ emission, Chemical technology, TP1-1185

Abstract

Luminescence methods for non-contact temperature monitoring have evolved through improvements of hardware and sensor materials. Future advances in this field rely on the development of multimodal sensing capabilities of temperature probes and extend the temperature range across which they operate. The family of Cr-doped oxides appears particularly promising and we review their luminescence characteristics in light of their application in non-contact measurements of temperature over the 5–300 K range. Multimodal sensing utilizes the intensity ratio of emission lines, their wavelength shift, and the scintillation decay time constant. We carried out systematic studies of the temperature-induced changes in the luminescence of the Cr3+-doped oxides Al2O3, Ga2O3, Y3Al5O12, and YAlO3. The mechanism responsible for the temperature-dependent luminescence characteristic is discussed in terms of relevant models. It is shown that the thermally-induced processes of particle exchange, governing the dynamics of Cr3+ ion excited state populations, require low activation energy. This then translates into tangible changes of a luminescence parameter with temperature. We compare different schemes of temperature sensing and demonstrate that Ga2O3-Cr is a promising material for non-contact measurements at cryogenic temperatures. A temperature resolution better than ±1 K can be achieved by monitoring the luminescence intensity ratio (40–140 K) and decay time constant (80–300 K range).

Published

2020

14. Golgi enrichment and proteomic analysis of developing Pinus radiata xylem by free-flow electrophoresis.

Author

Harriet T Parsons, Cristina S Weinberg, Lucy J Macdonald, Paul D Adams, Christopher J Petzold, Timothy J Strabala, Armin Wagner, and Joshua L Heazlewood

Subjects

Medicine, Science

Abstract

Our understanding of the contribution of Golgi proteins to cell wall and wood formation in any woody plant species is limited. Currently, little Golgi proteomics data exists for wood-forming tissues. In this study, we attempted to address this issue by generating and analyzing Golgi-enriched membrane preparations from developing xylem of compression wood from the conifer Pinus radiata. Developing xylem samples from 3-year-old pine trees were harvested for this purpose at a time of active growth and subjected to a combination of density centrifugation followed by free flow electrophoresis, a surface charge separation technique used in the enrichment of Golgi membranes. This combination of techniques was successful in achieving an approximately 200-fold increase in the activity of the Golgi marker galactan synthase and represents a significant improvement for proteomic analyses of the Golgi from conifers. A total of thirty known Golgi proteins were identified by mass spectrometry including glycosyltransferases from gene families involved in glucomannan and glucuronoxylan biosynthesis. The free flow electrophoresis fractions of enriched Golgi were highly abundant in structural proteins (actin and tubulin) indicating a role for the cytoskeleton during compression wood formation. The mass spectrometry proteomics data associated with this study have been deposited to the ProteomeXchange with identifier PXD000557.

Published

2013

15. Biochemical and structural characterization of a sphingomonad diarylpropane lyase for cofactorless deformylation

Author

Eugene Kuatsjah, Michael Zahn, Xiangyang Chen, Ryo Kato, Daniel J. Hinchen, Mikhail O. Konev, Rui Katahira, Christian Orr, Armin Wagner, Yike Zou, Stefan J. Haugen, Kelsey J. Ramirez, Joshua K. Michener, Andrew R. Pickford, Naofumi Kamimura, Eiji Masai, K. N. Houk, John E. McGeehan, and Gregg T. Beckham

Subjects

Multidisciplinary, Bacterial Proteins, Lyases, lignin, Stereoisomerism, Oxidoreductases, NTF-2, Sphingobium sp. SYK-6, Novosphingobium aromaticivorans, aromatic catabolism

Abstract

Lignin valorization is being intensely pursued via tandem catalytic depolymerization and biological funneling to produce single products. In many lignin depolymerization processes, aromatic dimers and oligomers linked by carbon–carbon bonds remain intact, necessitating the development of enzymes capable of cleaving these compounds to monomers. Recently, the catabolism of erythro -1,2-diguaiacylpropane-1,3-diol ( erythro -DGPD), a ring-opened lignin-derived β-1 dimer, was reported in Novosphingobium aromaticivorans . The first enzyme in this pathway, LdpA (formerly LsdE), is a member of the nuclear transport factor 2 (NTF-2)-like structural superfamily that converts erythro -DGPD to lignostilbene through a heretofore unknown mechanism. In this study, we performed biochemical, structural, and mechanistic characterization of the N. aromaticivorans LdpA and another homolog identified in Sphingobium sp. SYK-6, for which activity was confirmed in vivo. For both enzymes, we first demonstrated that formaldehyde is the C 1 reaction product, and we further demonstrated that both enantiomers of erythro -DGPD were transformed simultaneously, suggesting that LdpA, while diastereomerically specific, lacks enantioselectivity. We also show that LdpA is subject to a severe competitive product inhibition by lignostilbene. Three-dimensional structures of LdpA were determined using X-ray crystallography, including substrate-bound complexes, revealing several residues that were shown to be catalytically essential. We used density functional theory to validate a proposed mechanism that proceeds via dehydroxylation and formation of a quinone methide intermediate that serves as an electron sink for the ensuing deformylation. Overall, this study expands the range of chemistry catalyzed by the NTF-2-like protein family to a prevalent lignin dimer through a cofactorless deformylation reaction.

Published

2023

16. Structures of annexin A2-PS DNA complexes show dominance of hydrophobic interactions in phosphorothioate binding

Author

Malwina Hyjek-Składanowska, Brooke A Anderson, Vitaliy Mykhaylyk, Christian Orr, Armin Wagner, Jarosław T Poznański, Krzysztof Skowronek, Punit Seth, and Marcin Nowotny

Subjects

ddc:570, Genetics

Abstract

Nucleic acids research / Special publication xx, gkac774 (2022). doi:10.1093/nar/gkac774, The introduction of phosphorothioate (PS) linkages to the backbone of therapeutic nucleic acids substantially increases their stability and potency. It also affects their interactions with cellular proteins, but the molecular mechanisms that underlie this effect are poorly understood. Here, we report structural and biochemical studies of interactions between annexin A2, a protein that does not possess any known canonical DNA binding domains, and phosphorothioate-modified antisense oligonucleotides. We show that a unique mode of hydrophobic interactions between a sulfur atom of the phosphorothioate group and lysine and arginine residues account for the enhanced affinity of modified nucleic acid for the protein. Our results demonstrate that this mechanism of interaction is observed not only for nucleic acid-binding proteins but can also account for the association of PS oligonucleotides with other proteins. Using the anomalous diffraction of sulfur, we showed that preference for phosphorothioate stereoisomers is determined by the hydrophobic environment around the PS linkage that comes not only from protein but also from additional structural features within the ASO such as 5-Me groups on cytosine nucleobases., Published by Information Retrieval Ltd., London

Published

2023

17. Novel quaternary structures of the human prion protein globular domain

Author

Sonia M Vallabh, José Brandão-Neto, Maria Cristina Nonato, R. Talon, Leandro Oliveira Bortot, Armin Wagner, Stuart L. Schreiber, Frank von Delft, Eric Vallabh Minikel, Kamel El Omari, Andrew G. Reidenbach, Francesca A. Pavlovici, and V.L. Rangel

Subjects

Amyloid, Chemistry, Drug discovery, animal diseases, Disulfide bond, General Medicine, Crystallography, X-Ray, Biochemistry, Article, nervous system diseases, Domain (software engineering), Molecular dynamics, Protein Domains, Native state, Biophysics, Humans, PrPC Proteins, Prion protein, Protein Structure, Quaternary, Conformational isomerism

Abstract

Prion disease is caused by the misfolding of the cellular prion protein, PrPC, into a self-templating conformer, PrPSc. Nuclear magnetic resonance (NMR) and X-ray crystallography revealed the 3D structure of the globular domain of PrPC and the possibility of its dimerization via an interchain disulfide bridge that forms due to domain swap or by non-covalent association of two monomers. On the contrary, PrPSc is composed by a complex and heterogeneous ensemble of poorly defined conformations and quaternary arrangements that are related to different patterns of neurotoxicity. Targeting PrPC with molecules that stabilize the native conformation of its globular domain emerged as a promising approach to develop anti-prion therapies. One of the advantages of this approach is employing structure-based drug discovery methods to PrPC. Thus, it is essential to expand our structural knowledge about PrPC as much as possible to aid such drug discovery efforts. In this work, we report a crystallographic structure of the globular domain of human PrPC that shows a novel dimeric form and a novel oligomeric arrangement. We use molecular dynamics simulations to explore its structural dynamics and stability and discuss potential implications of these new quaternary structures to the conversion process.

Published

2021

18. Directional regulation of cytosolic PEPCK catalysis is mediated by competitive binding of anions

Author

Sarah A.E. Barwell, Ramona Duman, Armin Wagner, and Todd Holyoak

Subjects

Phosphoenolpyruvate, Anions, Biophysics, Cell Biology, Molecular Biology, Biochemistry, Binding, Competitive, Phosphoenolpyruvate Carboxykinase (ATP), Catalysis

Abstract

Phosphoenolpyruvate carboxykinase (PEPCK) is a well-characterized enzyme involved in primary glucose metabolism, responsible for catalyzing one of the key steps of gluconeogenesis. It is well demonstrated that PEPCK can efficiently catalyze the reversible interconversion of oxaloacetic acid (OAA) to phosphoenolpyruvate (PEP) in vitro, but the enzyme is typically ascribed a metabolic role that requires preferential catalysis in the direction of PEP synthesis in vivo. Here we present structural and functional data that demonstrate the preferential synthesis of PEP from OAA catalyzed by PEPCK in vivo is facilitated by anion-mediated enzyme inhibition that reduces enzyme activity more significantly in the direction of OAA synthesis than in the direction of PEP synthesis. From our studies we conclude that the specific binding of small, ubiquitous anions like chloride, present in millimolar concentrations under normal cellular conditions allows for metabolic control by restricting PEPCK to function in the direction of PEP synthesis.

Published

2022

19. Fixed-target serial femtosecond crystallography using in cellulo grown microcrystals

Author

Pontus Fischer, Alke Meents, Lars Redecke, Armin Wagner, Miriam Barthelmess, J.M. Lahey-Rudolph, R. Schonherr, and Carolin Seuring

Subjects

Diffraction, serial femtosecond crystallography, Materials science, business.operation, Synchrotron radiation, 02 engineering and technology, Biochemistry, law.invention, silicon chip, 03 medical and health sciences, roadrunner, law, ddc:530, General Materials Science, 030304 developmental biology, 0303 health sciences, Crystallography, fixed-target sfx, Resolution (electron density), General Chemistry, 021001 nanoscience & nanotechnology, Condensed Matter Physics, Laser, Research Papers, Synchrotron, intracellular protein crystals, Roadrunner, in cellulo crystallography, QD901-999, Femtosecond, 0210 nano-technology, business, Protein crystallization

Abstract

IUCrJ 8(4), 665 - 677 (2021). doi:10.1107/S2052252521005297, The crystallization of recombinant proteins in living cells is an exciting new approach in structural biology. Recent success has highlighted the need for fast and efficient diffraction data collection, optimally directly exposing intact crystal-containing cells to the X-ray beam, thus protecting the in cellulo crystals from environmental challenges. Serial femtosecond crystallography (SFX) at free-electron lasers (XFELs) allows the collection of detectable diffraction even from tiny protein crystals, but requires very fast sample exchange to utilize each XFEL pulse. Here, an efficient approach is presented for high-resolution structure elucidation using serial femtosecond in cellulo diffraction of micometre-sized crystals of the protein HEX-1 from the fungus Neurospora crassa on a fixed target. Employing the fast and highly accurate Roadrunner II translation-stage system allowed efficient raster scanning of the pores of micro-patterned, single-crystalline silicon chips loaded with living, crystal-containing insect cells. Compared with liquid-jet and LCP injection systems, the increased hit rates of up to 30% and reduced background scattering enabled elucidation of the HEX-1 structure. Using diffraction data from only a single chip collected within 12 min at the Linac Coherent Light Source, a 1.8 Å resolution structure was obtained with significantly reduced sample consumption compared with previous SFX experiments using liquid-jet injection. This HEX-1 structure is almost superimposable with that previously determined using synchrotron radiation from single HEX-1 crystals grown by sitting-drop vapour diffusion, validating the approach. This study demonstrates that fixed-target SFX using micro-patterned silicon chips is ideally suited for efficient in cellulo diffraction data collection using living, crystal-containing cells, and offers huge potential for the straightforward structure elucidation of proteins that form intracellular crystals at both XFELs and synchrotron sources., Published by Chester

Published

2021

20. Hinge disulfides in human IgG2 CD40 antibodies modulate receptor signaling by regulation of conformation and flexibility

Author

Christian M. Orr, Hayden Fisher, Xiaojie Yu, Claude H.-T. Chan, Yunyun Gao, Patrick J. Duriez, Steven G. Booth, Isabel Elliott, Tatyana Inzhelevskaya, Ian Mockridge, Christine A. Penfold, Armin Wagner, Martin J. Glennie, Ann L. White, Jonathan W. Essex, Arwen R. Pearson, Mark S. Cragg, and Ivo Tews

Subjects

Epitopes, Protein Conformation, Immunoglobulin G, Immunology, Antibodies, Monoclonal, Humans, General Medicine, Disulfides

Abstract

Antibodies protect from infection, underpin successful vaccines and elicit therapeutic responses in otherwise untreatable cancers and autoimmune conditions. The human IgG2 isotype displays a unique capacity to undergo disulfide shuffling in the hinge region, leading to modulation of its ability to drive target receptor signaling (agonism) in a variety of important immune receptors, through hitherto unexplained molecular mechanisms. To address the underlying process and reveal how hinge disulfide orientation affects agonistic activity, we generated a series of cysteine to serine exchange variants in the hinge region of the clinically relevant monoclonal antibody ChiLob7/4, directed against the key immune receptor CD40. We report how agonistic activity varies with disulfide pattern and is afforded by the presence of a disulfide crossover between F(ab) arms in the agonistic forms, independently of epitope, as observed in the determined crystallographic structures. This structural “switch” affects directly on antibody conformation and flexibility. Small-angle x-ray scattering and ensemble modeling demonstrated that the least flexible variants adopt the fewest conformations and evoke the highest levels of receptor agonism. This covalent change may be amenable for broad implementation to modulate receptor signaling in an epitope-independent manner in future therapeutics.

Published

2022

21. »Verehrter Parteigenosse Landfried!«

Author

Armin Wagner and Magnus Pahl

Subjects

General Earth and Planetary Sciences, General Environmental Science

Abstract

Zusammenfassung Vom Juli bis Dezember 2019 zeigte das Militärhistorische Museum der Bundeswehr (MHM) in Dresden eine Ausstellung anlässlich des 75. Jahrestages des Attentats auf Adolf Hitler und des geplanten Umsturzversuches vom 20. Juli 1944. Nach Publikation des Katalogs kamen Verdachtsmomente auf, einige der dort gezeigten Dokumente seien gefälscht. Prüfungen des Museums, unter anderem mit Unterstützung des Landeskriminalamtes Sachsen, bestätigten diesen Verdacht teilweise. Der Beitrag beschreibt, wie die entsprechenden Schriftstücke an das MHM kamen, warum sie für echt gehalten und in der Ausstellung präsentiert wurden und wie im Nachgang die Fälschung erkannt wurde. Er schließt mit knappen Überlegungen, was künftig daraus für den Erwerb von Museumsgut zu folgern ist.

Published

2021

22. Al2O3 co-doped with Cr3+ and Mn4+, a dual-emitter probe for multimodal non-contact luminescence thermometry

Author

Vasyl Hreb, Leonid Vasylechko, Iryna Lutsyuk, Lev-Ivan Bulyk, Andrzej Suchocki, Vitaliy Mykhaylyk, Yaroslav Zhydachevskyy, H. Kraus, and Armin Wagner

Subjects

Inorganic Chemistry, Range (particle radiation), Accuracy and precision, Materials science, business.industry, Resolution (electron density), Optoelectronics, Emission spectrum, Atmospheric temperature range, Luminescence, business, Ion, Common emitter

Abstract

Luminescence probes that facilitate multimodal non-contact measurements of temperature are of particular interest due to the possibility of cross-referencing results across different readout techniques. This intrinsic referencing is an essential addition that enhances accuracy and reliability of the technique. A further enhancement of sensor performance can be achieved by using two luminescent ions acting as independent emitters, thereby adding in-built redundancy to non-contact temperature sensing, using a single readout technique. In this study we combine both approaches by engineering a material with two luminescent ions that can be independently probed through different readout modes of non-contact temperature sensing. The approach was tested using Al2O3 co-doped with Cr3+ and Mn4+, exhibiting sharp emission lines due to 2E → 4A2 transitions. The temperature sensing performance was examined by measuring three characteristics: temperature-induced changes of the intensity ratio of the emission lines, their spectral position, and the luminescence decay time constant. The processes responsible for the changes with temperature of the measured luminescence characteristics are discussed in terms of relevant models. By comparing temperature resolutions achievable by different modes of temperature sensing it is established that in Al2O3-Cr,Mn spectroscopic methods provide the best measurement accuracy over a broad temperature range. A temperature resolution better than ±2.8 K can be achieved by monitoring the luminescence intensity ratio (40–145 K) and the spectral shift of the R-line of Mn4+ (145–300 K range).

Published

2021

23. Native de novo structural determinations of non-canonical nucleic acid motifs by X-ray crystallography at long wavelengths

Author

Yashu Zhang, Kamel El Omari, Armin Wagner, Dengguo Wei, Gary N. Parkinson, Ramona Duman, Shozeb Haider, and Sisi Liu

Subjects

AcademicSubjects/SCI00010, Biology, Crystallography, X-Ray, 010402 general chemistry, G-quadruplex, 01 natural sciences, 03 medical and health sciences, chemistry.chemical_compound, Narese/14, Structural Biology, Genetics, Humans, Nucleotide, Nucleotide Motifs, Nucleic acid structure, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Anomalous scattering, Nucleic acid structure determination, RNA, Telomere, Herpesvirus 1, Suid, 0104 chemical sciences, G-Quadruplexes, Crystallography, chemistry, Nucleic acid, RNA, Viral, DNA

Abstract

Obtaining phase information remains a formidable challenge for nucleic acid structure determination. The introduction of an X-ray synchrotron beamline designed to be tunable to long wavelengths at Diamond Light Source has opened the possibility to native de novo structure determinations by the use of intrinsic scattering elements. This provides opportunities to overcome the limitations of introducing modifying nucleotides, often required to derive phasing information. In this paper, we build on established methods to generate new tools for nucleic acid structure determinations. We report on the use of (i) native intrinsic potassium single-wavelength anomalous dispersion methods (K-SAD), (ii) use of anomalous scattering elements integral to the crystallization buffer (extrinsic cobalt and intrinsic potassium ions), (iii) extrinsic bromine and intrinsic phosphorus SAD to solve complex nucleic acid structures. Using the reported methods we solved the structures of (i) Pseudorabies virus (PRV) RNA G-quadruplex and ligand complex, (ii) PRV DNA G-quadruplex, and (iii) an i-motif of human telomeric sequence. Our results highlight the utility of using intrinsic scattering as a pathway to solve and determine non-canonical nucleic acid motifs and reveal the variability of topology, influence of ligand binding, and glycosidic angle rearrangements seen between RNA and DNA G-quadruplexes of the same sequence.

Published

2020

24. Structure and assembly of the S-layer in C. difficile

Author

Paola, Lanzoni-Mangutchi, Oishik, Banerji, Jason, Wilson, Anna, Barwinska-Sendra, Joseph A, Kirk, Filipa, Vaz, Shauna, O'Beirne, Arnaud, Baslé, Kamel, El Omari, Armin, Wagner, Neil F, Fairweather, Gillian R, Douce, Per A, Bullough, Robert P, Fagan, and Paula S, Salgado

Subjects

Bacterial Proteins, Cell Wall, Clostridioides difficile

Abstract

Many bacteria and archaea possess a two-dimensional protein array, or S-layer, that covers the cell surface and plays crucial roles in cell physiology. Here, we report the crystal structure of SlpA, the main S-layer protein of the bacterial pathogen Clostridioides difficile, and use electron microscopy to study S-layer organisation and assembly. The SlpA crystal lattice mimics S-layer assembly in the cell, through tiling of triangular prisms above the cell wall, interlocked by distinct ridges facing the environment. Strikingly, the array is very compact, with pores of only ~10 Å in diameter, compared to other S-layers (30-100 Å). The surface-exposed flexible ridges are partially dispensable for overall structure and assembly, although a mutant lacking this region becomes susceptible to lysozyme, an important molecule in host defence. Thus, our work gives insights into S-layer organisation and provides a basis for development of C. difficile-specific therapeutics.

Published

2021

25. Structure and function of the ROR2 cysteine-rich domain in vertebrate noncanonical WNT5A signaling

Author

Levi L. Blazer, Jarrett Adams, Ho H-Yh., Christian Siebold, S.C. Griffiths, Justin Tan, Sachdev S. Sidhu, and Armin Wagner

Subjects

Frizzled, biology, Chemistry, ROR2, medicine.disease, eye diseases, Receptor tyrosine kinase, Robinow syndrome, Cell biology, body regions, Extracellular, biology.protein, medicine, Receptor, Function (biology), Cysteine

Abstract

The receptor tyrosine kinase ROR2 mediates noncanonical WNT5A signaling to orchestrate tissue morphogenetic processes, and dysfunction of the pathway causes Robinow syndrome, Brachydactyly B and metastatic diseases. The domain(s) and mechanisms required for ROR2 function, however, remain unclear. We solved the crystal structure of the extracellular cysteine-rich (CRD) and Kringle (Kr) domains of ROR2 and found that, unlike other CRDs, the ROR2 CRD lacks the signature hydrophobic pocket that binds lipids/lipid-modified proteins, such as WNTs, suggesting a novel mechanism of receptor action. Functionally, we showed that the ROR2 CRD, but not other domains, is required and minimally sufficient to promote WNT5A signaling, and Robinow mutations in the CRD and the adjacent Kr alter ROR2 function. Moreover, we demonstrated that the activity of the ROR2 CRD requires Frizzled receptors. Thus, ROR2 acts via its CRD to potentiate the function of a receptor supercomplex that includes Frizzleds to transduce WNT5A signals.

Published

2021

26. Phosphorus and sulfur SAD phasing of the nucleic acid-bound DNA-binding domain of interferon regulatory factor 4

Author

Armin Wagner, A. Agnarelli, K. El Omari, R. Duman, and Erika J. Mancini

Subjects

experimental phasing, interferon regulatory factor 4, Response element, Biophysics, Crystallography, X-Ray, Biochemistry, DNA-binding protein, Protein Structure, Secondary, Research Communications, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Protein Domains, IRF4, Structural Biology, Transcription (biology), Nucleic Acids, Genetics, Humans, Molecular replacement, native SAD, 030304 developmental biology, 0303 health sciences, Binding Sites, Oligonucleotide, Phosphorus, DNA, DNA-binding domain, Condensed Matter Physics, Protein Structure, Tertiary, DNA-Binding Proteins, chemistry, 030220 oncology & carcinogenesis, Interferon Regulatory Factors, Nucleic acid, Sulfur

Abstract

Solution of the structure of the DNA-binding domain of interferon regulatory factor 4 bound to its interferon-stimulated response element by native intrinsic phosphorus and sulfur single-wavelength anomalous dispersion methods (native SAD) is described., Pivotal to the regulation of key cellular processes such as the transcription, replication and repair of DNA, DNA-binding proteins play vital roles in all aspects of genetic activity. The determination of high-quality structures of DNA-binding proteins, particularly those in complexes with DNA, provides crucial insights into the understanding of these processes. The presence in such complexes of phosphate-rich oligonucleotides offers the choice of a rapid method for the routine solution of DNA-binding proteins through the use of long-wavelength beamlines such as I23 at Diamond Light Source. This article reports the use of native intrinsic phosphorus and sulfur single-wavelength anomalous dispersion methods to solve the complex of the DNA-binding domain (DBD) of interferon regulatory factor 4 (IRF4) bound to its interferon-stimulated response element (ISRE). The structure unexpectedly shows three molecules of the IRF4 DBD bound to one ISRE. The sole reliance on native intrinsic anomalous scattering elements that belong to DNA–protein complexes renders the method of general applicability to a large number of such protein complexes that cannot be solved by molecular replacement or by other phasing methods.

Published

2021

27. Desolvation of the substrate-binding protein TauA dictates ligand specificity for the alkanesulfonate ABC importer TauABC

Author

Feng Qu, Kamel ElOmari, Armin Wagner, Alfonso De Simone, Konstantinos Beis, Qu, F., Elomari, K., Wagner, A., De Simone, A., Beis, K., and Medical Research Council (MRC)

Subjects

0301 basic medicine, Taurine, Ligands, 01 natural sciences, Biochemistry, Substrate Specificity, ABC transport protein, Mutant Protein, Structural Biology, ABC transport proteins, Escherichia coli Protein, WATER, Alkanesulfonate, 11 Medical and Health Sciences, Research Articles, Molecular Interactions, molecular dynamic, Escherichia coli Proteins, HYDRATION, Protein Transport, ESCHERICHIA-COLI, 03 Chemical Sciences, Crystallization, Life Sciences & Biomedicine, Protein Binding, Alkanesulfonates, Biochemistry & Molecular Biology, ATP-Binding Cassette Transporter, Protein Domain, Ligand, Molecular Dynamics Simulation, 010402 general chemistry, thermodynamic, 03 medical and health sciences, thermodynamics, Protein Domains, Escherichia coli, crystallography, Molecular Biology, Science & Technology, Binding Sites, Base Sequence, RECOGNITION, Binding Site, Computational Biology, Hydrogen Bonding, Cell Biology, 06 Biological Sciences, molecular dynamics, 0104 chemical sciences, MODEL, 030104 developmental biology, ATP-Binding Cassette Transporters, Mutant Proteins, Cell Membranes, Excitation & Transport, Carrier Protein, Carrier Proteins, Sulfur

Abstract

Under limiting sulfur availability, bacteria can assimilate sulfur from alkanesulfonates. Bacteria utilize ATP-binding cassette (ABC) transporters to internalise them for further processing to release sulfur. In gram-negative bacteria the TauABC and SsuABC ensure internalization, although, these two systems have common substrates, the former has been characterized as a taurine specific system. TauA and SsuA are substrate-binding proteins (SBPs) that bind and bring the alkanesulfonates to the ABC importer for transport. Here, we have determined the crystal structure of TauA and have characterized its thermodynamic binding parameters by isothermal titration calorimetry in complex with taurine and different alkanesulfonates. Our structures revealed that the coordination of the alkanesulfonates is conserved, with the exception of Asp205 that is absent from SsuA, but the thermodynamic parameters revealed a very high enthalpic penalty cost for binding of the other alkanesulfonates relative to taurine. Our molecular dynamic simulations indicated that the different levels of hydration of the binding site contributed to the selectivity for taurine over the other alkanesulfonates. Such selectivity mechanism is very likely to be employed by other SBPs of ABC transporters.

Published

2019

28. The morphogen Sonic hedgehog inhibits its receptor Patched by a pincer grasp mechanism

Author

Armin Wagner, Douglas F. Covey, Jan Steyaert, Rebekka A. Schwab, Els Pardon, Tomas Malinauskas, Rajat Rohatgi, Christian Siebold, Mark S.P. Sansom, A.F. Rudolf, Kamel El Omari, Ramona Duman, Mingxing Qian, C. Kowatsch, T. Bertie Ansell, B. Bishop, Maia Kinnebrew, Department of Bio-engineering Sciences, and Structural Biology Brussels

Subjects

Patched, Models, Molecular, endocrine system, Protein Conformation, Article, 03 medical and health sciences, Mice, Extracellular, Animals, Humans, Hedgehog Proteins, Sonic hedgehog, Receptor, Molecular Biology, Hedgehog, 030304 developmental biology, 0303 health sciences, biology, Chemistry, 030302 biochemistry & molecular biology, Cell Biology, Single-Domain Antibodies, Sterol transport, Cell biology, Patched-1 Receptor, Cholesterol, HEK293 Cells, PTCH1, Gene Expression Regulation, biology.protein, NIH 3T3 Cells, lipids (amino acids, peptides, and proteins), Morphogen, Protein Binding

Abstract

Hedgehog (HH) ligands, classical morphogens that pattern embryonic tissues in all animals, are covalently coupled to two lipids—a palmitoyl group at the N terminus and a cholesteroyl group at the C terminus. While the palmitoyl group binds and inactivates Patched 1 (PTCH1), the main receptor for HH ligands, the function of the cholesterol modification has remained mysterious. Using structural and biochemical studies, along with reassessment of previous cryo-electron microscopy structures, we find that the C-terminal cholesterol attached to Sonic hedgehog (Shh) binds the first extracellular domain of PTCH1 and promotes its inactivation, thus triggering HH signaling. Molecular dynamics simulations show that this interaction leads to the closure of a tunnel through PTCH1 that serves as the putative conduit for sterol transport. Thus, Shh inactivates PTCH1 by grasping its extracellular domain with two lipidic pincers, the N-terminal palmitate and the C-terminal cholesterol, which are both inserted into the PTCH1 protein core. Cholesterol can function as both a substrate and an inhibitor of the Hedgehog receptor Patched. Structural analysis and molecular dynamics simulations reveal that cholesterol inhibits Patched by inserting into its extracellular domain

Published

2019

29. Jörn Happel, Der Ost-Experte. Gustav Hilger – Diplomat im Zeitalter der Extreme, Paderborn [u. a.]: Schöningh 2018, 533 S., EUR 68,00 [ISBN 978‑3‑506‑78609‑8]

Author

Armin Wagner

Subjects

General Earth and Planetary Sciences, General Environmental Science

Published

2019

30. Molecular mechanism of Mad1 kinetochore targeting by phosphorylated Bub1

Author

Stefan M.V. Freund, Conny Wing-Heng Yu, Elyse S Fischer, David Barford, Dom Bellini, Stephen H. McLaughlin, Armin Wagner, Christian M. Orr, Fischer, Elyse S [0000-0001-8746-039X], Yu, Conny WH [0000-0002-6478-5762], Bellini, Dom [0000-0003-0576-3413], McLaughlin, Stephen H [0000-0001-9135-6253], Orr, Christian M [0000-0002-6137-8969], Barford, David [0000-0001-8810-950X], and Apollo - University of Cambridge Repository

Subjects

Mad1, Mitotic checkpoint complex, Protein domain, BUB1, Cell Cycle Proteins, Spindle Apparatus, Cell cycle, Biochemistry, Spindle assembly checkpoint, Article, 03 medical and health sciences, 0302 clinical medicine, Structural Biology, Chromosome Segregation, Genetics, Phosphorylation, Kinetochores, Molecular Biology, Metaphase, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries), ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, 0303 health sciences, Chemistry, Kinetochore, Kinase, Articles, Cell biology, Spindle checkpoint, Mad2 Proteins, Bub1, 030217 neurology & neurosurgery, Signal Transduction

Abstract

During metaphase, in response to improper kinetochore‐microtubule attachments, the spindle assembly checkpoint (SAC) activates the mitotic checkpoint complex (MCC), an inhibitor of the anaphase‐promoting complex/cyclosome (APC/C). This process is orchestrated by the kinase Mps1, which initiates the assembly of the MCC onto kinetochores through a sequential phosphorylation‐dependent signalling cascade. The Mad1‐Mad2 complex, which is required to catalyse MCC formation, is targeted to kinetochores through a direct interaction with the phosphorylated conserved domain 1 (CD1) of Bub1. Here, we present the crystal structure of the C‐terminal domain of Mad1 (Mad1CTD) bound to two phosphorylated Bub1CD1 peptides at 1.75 Å resolution. This interaction is mediated by phosphorylated Bub1 Thr461, which not only directly interacts with Arg617 of the Mad1 RLK (Arg‐Leu‐Lys) motif, but also directly acts as an N‐terminal cap to the CD1 α‐helix dipole. Surprisingly, only one Bub1CD1 peptide binds to the Mad1 homodimer in solution. We suggest that this stoichiometry is due to inherent asymmetry in the coiled‐coil of Mad1CTD and has implications for how the Mad1‐Bub1 complex at kinetochores promotes efficient MCC assembly., Activation of the mitotic checkpoint complex (MCC) is orchestrated by a sequential phosphorylation‐dependent signalling cascade. This study reveals the molecular mechanism for kinetochore targeting of the Mad1‐Mad2 complex.

Published

2021

31. X-ray tomographic reconstruction and segmentation pipeline for the long-wavelength macromolecular crystallography beamline at Diamond Light Source

Author

Kazimir Wanelik, Nicola Wadeson, Mark Basham, Vitaliy Mykhaylyk, Ramona Duman, Armin Wagner, and Daniil Kazantsev

Subjects

Nuclear and High Energy Physics, Data processing, iterative reconstruction, Radiation, Tomographic reconstruction, Computer science, Pipeline (computing), segmentation, high-performance computing, Iterative reconstruction, 01 natural sciences, Thresholding, Research Papers, 010309 optics, Beamline, 0103 physical sciences, absorption correction, Segmentation, Tomography, 010306 general physics, long-wavelength X-ray crystallography, Instrumentation, Algorithm

Abstract

Automatic segmentation methods developed for tomography data collected on macromolecular crystallography beamline I23, Diamond Light Source, to assist with absorption corrections for very long wavelengths X-ray diffraction data are presented., In this paper a practical solution for the reconstruction and segmentation of low-contrast X-ray tomographic data of protein crystals from the long-wavelength macromolecular crystallography beamline I23 at Diamond Light Source is provided. The resulting segmented data will provide the path lengths through both diffracting and non-diffracting materials as basis for analytical absorption corrections for X-ray diffraction data taken in the same sample environment ahead of the tomography experiment. X-ray tomography data from protein crystals can be difficult to analyse due to very low or absent contrast between the different materials: the crystal, the sample holder and the surrounding mother liquor. The proposed data processing pipeline consists of two major sequential operations: model-based iterative reconstruction to improve contrast and minimize the influence of noise and artefacts, followed by segmentation. The segmentation aims to partition the reconstructed data into four phases: the crystal, mother liquor, loop and vacuum. In this study three different semi-automated segmentation methods are experimented with by using Gaussian mixture models, geodesic distance thresholding and a novel morphological method, RegionGrow, implemented specifically for the task. The complete reconstruction-segmentation pipeline is integrated into the MPI-based data analysis and reconstruction framework Savu, which is used to reduce computation time through parallelization across a computing cluster and makes the developed methods easily accessible.

Published

2020

32. Experimental phasing with vanadium and application to nucleotide-binding membrane proteins

Author

Hok-Sau Kwong, Maike Bublitz, Claus Olesen, Vitaliy Mykhaylyk, Armin Wagner, Jesper V. Møller, Konstantinos Beis, Nada Mohamad, R. Duman, Kiran Bountra, Katja Schlegel, Maria Romano, and Kamel El Omari

Subjects

experimental phasing, RNase P, Vanadium, chemistry.chemical_element, membrane proteins, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Protein structure, General Materials Science, Vanadate, lcsh:Science, Integral membrane protein, 030304 developmental biology, 0303 health sciences, biology, Chemistry, Endoplasmic reticulum, fungi, Active site, food and beverages, General Chemistry, Condensed Matter Physics, Combinatorial chemistry, Research Papers, Membrane protein, biology.protein, vanadium, lcsh:Q, 030217 neurology & neurosurgery

Abstract

Crystal structure determination of membrane proteins can be challenging. Here, the use of vanadium phasing as an alternative experimental phasing method is described., The structure determination of soluble and membrane proteins can be hindered by the crystallographic phase problem, especially in the absence of a suitable homologous structure. Experimental phasing is the method of choice for novel structures; however, it often requires heavy-atom derivatization, which can be difficult and time-consuming. Here, a novel and rapid method to obtain experimental phases for protein structure determination by vanadium phasing is reported. Vanadate is a transition-state mimic of phosphoryl-transfer reactions and it has the advantage of binding specifically to the active site of numerous enzymes catalyzing this reaction. The applicability of vanadium phasing has been validated by determining the structures of three different protein–vanadium complexes, two of which are integral membrane proteins: the rabbit sarcoplasmic reticulum Ca2+-ATPase, the antibacterial peptide ATP-binding cassette transporter McjD from Escherichia coli and the soluble enzyme RNAse A from Bos taurus. Vanadium phasing was successful even at low resolution and despite severe anisotropy in the data. This method is principally applicable to a large number of proteins, representing six of the seven Enzyme Commission classes. It relies exclusively on the specific chemistry of the protein and it does not require any modifications, making it a very powerful addition to the phasing toolkit. In addition to the phasing power of this technique, the protein–vanadium complexes also provide detailed insights into the reaction mechanisms of the studied proteins.

Published

2020

33. Structure and assembly of the S-layer determine virulence in C. difficile

Author

Gill Douce, Robert P. Fagan, P. Lanzoni-Mangutchi, Joseph A. Kirk, Armin Wagner, Per A. Bullough, A. Basle, A. Barwinska-Sendra, J. Wilson, Paula S. Salgado, Oishik Banerji, S. O'Beirne, F. Vaz, Neil F. Fairweather, and K. El Omari

Subjects

Antibiotic resistance, Protein microarray, Virulence, Computational biology, Disease, Biology, C difficile, S-layer, Pathogen, Function (biology)

Abstract

Many bacteria and archaea possess a cell surface layer – S-layer – made of a 2D protein array that covers the entire cell. As the outermost component of the cell envelope, S-layers play crucial roles in many aspects of cell physiology. Importantly, many clinically relevant bacterial pathogens possess a distinct S-layer that forms an initial interface with the host, making it a potential target for development of species-specific antimicrobials. Targeted therapeutics are particularly important for antibiotic resistant pathogens such as Clostridioides difficile, the most frequent cause of hospital acquired diarrhea, which relies on disruption of normal microbiota through antibiotic usage. Despite the ubiquity of S-layers, only partial structural information from a very limited number of species is available and their function and organization remains poorly understood. Here we report the first complete atomic level structure and in situ assembly model of an S-layer from a bacterial pathogen and reveal its role in disease severity. SlpA, the main C. difficile S-layer protein, assembles through tiling of triangular prisms abutting the cell wall, interlocked by distinct ridges facing the environment. This forms a tightly packed array, unlike the more porous S-layer models previously described. We report that removing one of the SlpA ridge features dramatically reduces disease severity, despite being dispensable for overall SlpA structure and S-layer assembly. Remarkably, the effect on disease severity is independent of toxin production and bacterial colonization within the mouse model of disease. Our work combines X-ray and electron crystallography to reveal a novel S-layer organization in atomic detail, highlighting the need for multiple technical approaches to obtain structural information on these paracrystalline arrays. These data also establish a direct link between specific structural elements of S-layer and virulence for the first time, in a crucial paradigm shift in our understanding of C. difficile disease, currently largely attributed to the action of potent toxins. This work highlights the crucial role of S-layers in pathogenicity and the importance of detailed structural information for providing new therapeutic avenues, targeting the S-layer. Understanding the interplay between S-layer and other virulence factors will further enhance our ability to tackle pathogens carrying an S-layer. We anticipate that this work provides a solid basis for development of new, C. difficile-specific therapeutics, targeting SlpA structure and S-layer assembly to reduce the healthcare burden of these infections.

Published

2020

34. K2P channel C-type gating involves asymmetric selectivity filter order-disorder transitions

Author

Andrew M. Natale, Daniel L. Minor, Michael Grabe, Armin Wagner, Sara Capponi, Fayal Abderemane-Ali, David Crottès, Ramona Duman, John M. Rosenberg, and Marco Lolicato

Subjects

Potassium, Biophysics, chemistry.chemical_element, Gating, Biochemistry, 03 medical and health sciences, Molecular dynamics, 0302 clinical medicine, Ion binding, Structural Biology, Research Articles, 030304 developmental biology, K2p channel, 0303 health sciences, Multidisciplinary, Anomalous scattering, Chemistry, Hydrogen bond, Neurosciences, SciAdv r-articles, Biological Sciences, Potassium channel, Electrophysiology, Transmembrane domain, Physical Sciences, Chemical Sciences, Selectivity, 030217 neurology & neurosurgery, Research Article

Abstract

The innately heterodimeric K2P filter permits two C-type gating mechanisms, pinching and dilation, to operate in one channel., K2P potassium channels regulate cellular excitability using their selectivity filter (C-type) gate. C-type gating mechanisms, best characterized in homotetrameric potassium channels, remain controversial and are attributed to selectivity filter pinching, dilation, or subtle structural changes. The extent to which such mechanisms control C-type gating of innately heterodimeric K2Ps is unknown. Here, combining K2P2.1 (TREK-1) x-ray crystallography in different potassium concentrations, potassium anomalous scattering, molecular dynamics, and electrophysiology, we uncover unprecedented, asymmetric, potassium-dependent conformational changes that underlie K2P C-type gating. These asymmetric order-disorder transitions, enabled by the K2P heterodimeric architecture, encompass pinching and dilation, disrupt the S1 and S2 ion binding sites, require the uniquely long K2P SF2-M4 loop and conserved “M3 glutamate network,” and are suppressed by the K2P C-type gate activator ML335. These findings demonstrate that two distinct C-type gating mechanisms can operate in one channel and underscore the SF2-M4 loop as a target for K2P channel modulator development.

Published

2020

35. Multimodal Non-Contact Luminescence Thermometry with Cr-Doped Oxides

Author

H. Kraus, Vitaliy Mykhaylyk, Armin Wagner, V. Tsiumra, Andrzej Suchocki, Andriy Luchechko, and Yaroslav Zhydachevskyy

Subjects

Materials science, wavelength shift thermometry, non-contact luminescence thermometry, 02 engineering and technology, Activation energy, 010402 general chemistry, lcsh:Chemical technology, 01 natural sciences, Biochemistry, Article, Analytical Chemistry, Ion, Cr3+ emission, lcsh:TP1-1185, Emission spectrum, Electrical and Electronic Engineering, luminescence decay thermometry, Instrumentation, Scintillation, Range (particle radiation), business.industry, Atmospheric temperature range, 021001 nanoscience & nanotechnology, Atomic and Molecular Physics, and Optics, 0104 chemical sciences, Excited state, Optoelectronics, 0210 nano-technology, Luminescence, business, intensity ratio thermometry

Abstract

Luminescence methods for non-contact temperature monitoring have evolved through improvements of hardware and sensor materials. Future advances in this field rely on the development of multimodal sensing capabilities of temperature probes and extend the temperature range across which they operate. The family of Cr-doped oxides appears particularly promising and we review their luminescence characteristics in light of their application in non-contact measurements of temperature over the 5&ndash, 300 K range. Multimodal sensing utilizes the intensity ratio of emission lines, their wavelength shift, and the scintillation decay time constant. We carried out systematic studies of the temperature-induced changes in the luminescence of the Cr3+-doped oxides Al2O3, Ga2O3, Y3Al5O12, and YAlO3. The mechanism responsible for the temperature-dependent luminescence characteristic is discussed in terms of relevant models. It is shown that the thermally-induced processes of particle exchange, governing the dynamics of Cr3+ ion excited state populations, require low activation energy. This then translates into tangible changes of a luminescence parameter with temperature. We compare different schemes of temperature sensing and demonstrate that Ga2O3-Cr is a promising material for non-contact measurements at cryogenic temperatures. A temperature resolution better than &plusmn, 1 K can be achieved by monitoring the luminescence intensity ratio (40&ndash, 140 K) and decay time constant (80&ndash, 300 K range).

Published

2020

36. Author response: The architecture of EMC reveals a path for membrane protein insertion

Author

Duccio Malinverni, Ramanujan S. Hegde, Robert J. Keenan, John P. O’Donnell, Elizabeth A. Miller, Szymon Juszkiewicz, Ben P. Phillips, Armin Wagner, and Yuichi Yagita

Subjects

Membrane protein, Computer science, Path (graph theory), Architecture, Topology

Published

2020

37. The architecture of EMC reveals a path for membrane protein insertion

Author

Duccio Malinverni, John P. O’Donnell, Armin Wagner, Ben P. Phillips, Robert J. Keenan, Ramanujan S. Hegde, Elizabeth A. Miller, Szymon Juszkiewicz, Yuichi Yagita, O'Donnell, John P [0000-0002-0571-3603], Phillips, Ben P [0000-0001-9117-4695], Juszkiewicz, Szymon [0000-0002-3361-7264], Wagner, Armin [0000-0001-8995-7324], Keenan, Robert J [0000-0003-1466-0889], Miller, Elizabeth A [0000-0002-1033-8369], Hegde, Ramanujan S [0000-0001-8338-852X], and Apollo - University of Cambridge Repository

Subjects

QH301-705.5, Structural Biology and Molecular Biophysics, Science, chemical biology, membrane proteins, General Biochemistry, Genetics and Molecular Biology, Cytosol, Protein Domains, Biochemistry and Chemical Biology, None, molecular biophysics, biochemistry, structural biology, Humans, chaperone, Biology (General), Integral membrane protein, Membrane insertion, General Immunology and Microbiology, biology, Chemistry, General Neuroscience, Endoplasmic reticulum, General Medicine, Transmembrane domain, endoplasmic reticulum, HEK293 Cells, Membrane protein, Structural biology, Chaperone (protein), biology.protein, Biophysics, Medicine, Organelle biogenesis, organelle biogenesis, Hydrophobic and Hydrophilic Interactions, SEC Translocation Channels, Biogenesis, Research Article

Abstract

Funder: Boehringer Ingelheim Fonds; FundRef: http://dx.doi.org/10.13039/501100001645, Funder: Naito Foundation; FundRef: http://dx.doi.org/10.13039/100007428, Funder: Japanese Biochemical Society, Approximately 25% of eukaryotic genes code for integral membrane proteins that are assembled at the endoplasmic reticulum. An abundant and widely conserved multi-protein complex termed EMC has been implicated in membrane protein biogenesis, but its mechanism of action is poorly understood. Here, we define the composition and architecture of human EMC using biochemical assays, crystallography of individual subunits, site-specific photocrosslinking, and cryo-EM reconstruction. Our results suggest that EMC's cytosolic domain contains a large, moderately hydrophobic vestibule that can bind a substrate's transmembrane domain (TMD). The cytosolic vestibule leads into a lumenally-sealed, lipid-exposed intramembrane groove large enough to accommodate a single substrate TMD. A gap between the cytosolic vestibule and intramembrane groove provides a potential path for substrate egress from EMC. These findings suggest how EMC facilitates energy-independent membrane insertion of TMDs, explain why only short lumenal domains are translocated by EMC, and constrain models of EMC's proposed chaperone function.

Published

2020

38. High-resolution mapping of metal ions reveals principles of surface layer assembly in Caulobacter crescentus cells

Author

Armin Wagner, Phillip J. Stansfeld, Ramona Duman, Kamel El Omari, Dimitrios Kolokouris, Andriko von Kügelgen, Jan Löwe, Andreas Kjaer, Danguole Kureisaite-Ciziene, Matthew Herdman, Tanmay A.M. Bharat, and Elspeth F. Garman

Subjects

Models, Molecular, Materials science, Protein Conformation, Cryo-electron microscopy, Metal ions in aqueous solution, Molecular Dynamics Simulation, Ion, Molecular dynamics, X-Ray Diffraction, Structural Biology, Caulobacter crescentus, QD, Surface layer, Molecular Biology, Ions, Membrane Glycoproteins, biology, Protein Stability, QH, Cell Membrane, Cryoelectron Microscopy, Resolution (electron density), biology.organism_classification, QP, QR, Biophysics, Calcium, Protein Multimerization, S-layer

Abstract

Summary Surface layers (S-layers) are proteinaceous crystalline coats that constitute the outermost component of most prokaryotic cell envelopes. In this study, we have investigated the role of metal ions in the formation of the Caulobacter crescentus S-layer using high-resolution structural and cell biology techniques, as well as molecular simulations. Utilizing optical microscopy of fluorescently tagged S-layers, we show that calcium ions facilitate S-layer lattice formation and cell-surface binding. We report all-atom molecular dynamics simulations of the S-layer lattice, revealing the importance of bound metal ions. Finally, using electron cryomicroscopy and long-wavelength X-ray diffraction experiments, we mapped the positions of metal ions in the S-layer at near-atomic resolution, supporting our insights from the cellular and simulations data. Our findings contribute to the understanding of how C. crescentus cells form a regularly arranged S-layer on their surface, with implications on fundamental S-layer biology and the synthetic biology of self-assembling biomaterials.

Published

2022

39. The Long-wavelength Macromolecular Crystallography I23 at Diamond Light Source

Author

Vinay Grama, Armin Wagner, Vitaliy Mykhaylykh, Kamel El Omari, and Ramona Duman

Subjects

0301 basic medicine, 03 medical and health sciences, Long wavelength, 030104 developmental biology, Light source, Materials science, business.industry, Macromolecular crystallography, engineering, Diamond, Optoelectronics, engineering.material, business

Published

2018

40. Characterisation of tungstate and molybdate crystals ABO4 (A = Ca, Sr, Zn, Cd; B = W, Mo) for luminescence lifetime cryothermometry

Author

Yaroslav Zhydachevskyy, V. Tsiumra, H.J. Kim, Nivin M. Ahmed, V. Mokina, Vitaliy Mykhaylyk, H. Kraus, and Armin Wagner

Subjects

010302 applied physics, Materials science, Exciton, Kinetics, Analytical chemistry, 02 engineering and technology, Atmospheric temperature range, Molybdate, 021001 nanoscience & nanotechnology, 01 natural sciences, chemistry.chemical_compound, chemistry, Tungstate, Excited state, 0103 physical sciences, Radiative transfer, General Materials Science, 0210 nano-technology, Luminescence

Abstract

Luminescence lifetime thermometry for remote temperature monitoring of cryogenic objects requires materials that exhibit a suitably large change of the luminescence kinetics at low temperatures. Results of systematic studies of the temperature-induced changes in the luminescence of tungstates and molybdates with the general formula ABO4 (A = Ca, Sr, Zn, Cd; B = W, Mo) over the 4.5–300 K temperature range are summarized. It is shown through analysing changes of the emission and excitation spectra, as well as the decay kinetics, that in these materials the luminescence is due to the emission of self-trapped excitons, a process that exhibits strong temperature dependence. The main emphasis of the study is on establishing the factors that determine the character of the temperature dependence of the luminescence decay time constant. We discuss our findings in terms of a model that analyses the dynamics of radiative and non-radiative transitions between the excited and ground states of the emission center. Two thermally activated processes drive the observed changes. The first is the non-radiative decay of excited states, resulting in a decrease of the luminescence decay time constant at high temperatures. Additionally it is demonstrated that in molybdates and tungstates the fine splitting of the excited state facilitates a second mechanism for thermally activated exchange of charged carriers between the two split levels. This has a noticeable effect on the dynamics of the radiative decay at low temperatures. We established that the sensitivity of the luminescence lifetime to temperature changes can be estimated by using information on the energy structure of materials. It is concluded that within tungstates and molybdates under study SrWO4 is the most promising material for application in luminescence lifetime cryothermometry.

Published

2018

41. Structural basis for the glycosyltransferase activity of the Salmonella effector SseK3

Author

Regina A. Günster, Teresa L. M. Thurston, Kamel El Omari, Armin Wagner, Luigi Martino, Katrin Rittinger, Diego Esposito, and Wellcome Trust

Subjects

CONFORMATIONAL-CHANGES, 0301 basic medicine, HOST, Arginine, PROTEIN, GT-A family, glycosyltransferase, Biochemistry, Protein structure, arginine modification, GLCNACYLATION, CRYSTAL-STRUCTURE, III SECRETION SYSTEM, chemistry.chemical_classification, biology, Effector, Chemistry, bacterial effectors, Salmonella enterica, 11 Medical And Health Sciences, CLOSTRIDIUM-DIFFICILE TOXIN, Ligand (biochemistry), SseK3, ESCHERICHIA-COLI, 03 Chemical Sciences, Life Sciences & Biomedicine, Biochemistry & Molecular Biology, GLUCOSYLTRANSFERASE ACTIVITY, 03 medical and health sciences, Glycosyltransferase, bacterial toxin, enzyme mechanism, arginine-modification, structural analysis, protein structure, Molecular Biology, X-ray crystallography, Science & Technology, 030102 biochemistry & molecular biology, Active site, Isothermal titration calorimetry, Cell Biology, 06 Biological Sciences, UDP-GlcNAc, 030104 developmental biology, Enzyme, glycosyltransferase type-A, glycosyltransgerase type-A, biology.protein, DEATH DOMAIN

Abstract

The Salmonella secreted effector SseK3 translocates into host cells, targeting innate immune responses including NF-κB activation. SseK3 is a glycosyltransferase that transfers an N-acetylglucosamine (GlcNAc) moiety onto the guanidino group of a target arginine, modulating host cell function. However, a lack of structural information has precluded elucidation of the molecular mechanisms in arginine and GlcNAc selection. We report here the crystal structure of SseK3 in its apo form and in complex with hydrolysed UDP-GlcNAc. SseK3 possesses the typical glycosyltransferase type-A (GT-A)-family fold and the metal-coordinating DXD motif essential for ligand binding and enzymatic activity. Several conserved residues were essential for arginine-GlcNAcylation and SseK3-mediated inhibition of NF-κB activation. Isothermal titration calorimetry revealed SseK3's preference for manganese coordination. The pattern of interactions in the substrate-bound SseK3 structure explained the selection of the primary ligand. Structural re-arrangement of the C-terminal residues upon ligand binding was crucial for SseK3's catalytic activity and NMR analysis indicated that SseK3 has limited UDP-GlcNAc hydrolysis activity. The release of free N-acetyl α-D-glucosamine, and the presence of the same molecule in the SseK3 active site, classified it as a retaining glycosyltransferase. A glutamate residue in the active site suggested a double-inversion mechanism for the arginine N-glycosylation reaction. Homology models of SseK1, SseK2, and the Escherichia coli orthologue NleB1, reveal differences in the surface electrostatic charge distribution possibly accounting for their diverse activities. This first structure of a retaining GT-A arginine N-glycosyltransferase provides an important step towards a better understanding of this enzyme class and their roles as bacterial effectors.

Published

2018

42. K2PChannel C-Type Gating Involves Asymmetric Selectivity Filter Order-Disorder Transitions

Author

Sara Capponi, Daniel L. Minor, Armin Wagner, David Crottès, John M. Rosenberg, Andrew M. Natale, Fayal Abderemane-Ali, Ramona Duman, Marco Lolicato, and Michael Grabe

Subjects

Physics, Combinatorics, Physical Sciences, Chemical Sciences, Biophysics, Selectivity filter, Order (group theory), Gating, Biological Sciences

Abstract

Author(s): Natale, Andrew M; Lolicato, Marco Gaetano Lorenz; Abderemane-Ali, Fayal; Crottes, David; Capponi, Sara; Duman, Ramona; Wagner, Armin; Rosenberg, John M; Grabe, Michael; Minor, Daniel L

Published

2021

43. Accurate Bond Lengths to Hydrogen Atoms from Single-Crystal X-ray Diffraction by Including Estimated Hydrogen ADPs and Comparison to Neutron and QM/MM Benchmarks

Author

Birger Dittrich, Jens Lübben, Ralf Flaig, Peter Luger, Stefan Mebs, and Armin Wagner

Subjects

Diffraction, Stucture Elucidation Methods | Hot Paper, Neutron diffraction, 010402 general chemistry, 010403 inorganic & nuclear chemistry, 01 natural sciences, Molecular physics, Catalysis, QM/MM, neutron diffraction, Molecule, Neutron, density functional theory, amino acids, Full Paper, Scattering, Chemistry, structure elucidation, Organic Chemistry, General Chemistry, Full Papers, X-ray diffraction, 0104 chemical sciences, Bond length, Crystallography, X-ray crystallography

Abstract

Amino acid structures are an ideal test set for method‐development studies in crystallography. High‐resolution X‐ray diffraction data for eight previously studied genetically encoding amino acids are provided, complemented by a non‐standard amino acid. Structures were re‐investigated to study a widely applicable treatment that permits accurate X−H bond lengths to hydrogen atoms to be obtained: this treatment combines refinement of positional hydrogen‐atom parameters with aspherical scattering factors with constrained “TLS+INV” estimated hydrogen anisotropic displacement parameters (H‐ADPs). Tabulated invariom scattering factors allow rapid modeling without further computations, and unconstrained Hirshfeld atom refinement provides a computationally demanding alternative when database entries are missing. Both should incorporate estimated H‐ADPs, as free refinement frequently leads to over‐parameterization and non‐positive definite H‐ADPs irrespective of the aspherical scattering model used. Using estimated H‐ADPs, both methods yield accurate and precise X−H distances in best quantitative agreement with neutron diffraction data (available for five of the test‐set molecules). This work thus solves the last remaining problem to obtain such results more frequently. Density functional theoretical QM/MM computations are able to play the role of an alternative benchmark to neutron diffraction.

Published

2017

44. Long-wavelength macromolecular crystallography – First successful native SAD experiment close to the sulfur edge

Author

O. Aurelius, Armin Wagner, K. El Omari, Vitaliy Mykhaylyk, and Ramona Duman

Subjects

0301 basic medicine, Nuclear and High Energy Physics, Phase (waves), engineering.material, 010403 inorganic & nuclear chemistry, 01 natural sciences, Article, 03 medical and health sciences, Optics, Instrumentation, Macromolecular crystallography, Data processing, Crystallographic phase problem, Anomalous scattering, business.industry, Chemistry, Diamond, Soft X-rays, Phaser, 0104 chemical sciences, X-ray diffraction, Wavelength, Sulfur SAD, 030104 developmental biology, Beamline, X-ray crystallography, engineering, business

Abstract

Phasing of novel macromolecular crystal structures has been challenging since the start of structural biology. Making use of anomalous diffraction of natively present elements, such as sulfur and phosphorus, for phasing has been possible for some systems, but hindered by the necessity to access longer X-ray wavelengths in order to make most use of the anomalous scattering contributions of these elements. Presented here are the results from a first successful experimental phasing study of a macromolecular crystal structure at a wavelength close to the sulfur K edge. This has been made possible by the in-vacuum setup and the long-wavelength optimised experimental setup at the I23 beamline at Diamond Light Source. In these early commissioning experiments only standard data collection and processing procedures have been applied, in particular no dedicated absorption correction has been used. Nevertheless the success of the experiment demonstrates that the capability to extract phase information can be even further improved once data collection protocols and data processing have been optimised.

Published

2017

45. Enabling Learning Experiences for Visually Impaired Children by Interaction Design

Author

Peter Fikar, Georg Kaindl, Roman Ganhör, Florian Güldenpfennig, and Armin Wagner

Subjects

Interactivity, Tangible computing, Human–computer interaction, Visually impaired, Computer science, Cognition, Interaction design, Set (psychology), Affordance, Haptic technology

Abstract

Interaction design and tangible computing offer rich opportunities for supporting children with impairments by means of enhanced therapeutic toys and educational materials. In order to explore how technology can be utilized to meet special requirements in the education of visually impaired children (and teenagers), we set up a practice-based research project at a special health center and school for the blind. Drawing on a number of design experiments involving educators and affected children, we came up with design proposals that enabled instructive (sensory) experiences despite their impairments in the sensory system. We describe two interactive prototypes in detail – a tangible color-picker toy, that we named The Cuebe, and an Audio-Tactile Map designed for e-learning – and show how they can support children in building new skills by augmenting physical properties and affordances. In both prototypes, tactility, haptics, and interactivity were crucial features, since all experiences originated at the fingertips and then unfolded higher-level sensory and cognitive processes. Moreover, the prototypes were also characterized by a high degree of open-endedness and customizability in their design, allowing educators to incorporate them in flexible ways to meet the needs of the children.

Published

2019

46. Importance of potassium ions for ribosome structure and function revealed by long-wavelength X-ray diffraction

Author

R. Duman, Gulnara Yusupova, Armin Wagner, A. Rozov, Marat Yusupov, Vitaliy Mykhaylyk, Kamel El Omari, I. Khusainov, Eric Westhof, Centre National de la Recherche Scientifique (CNRS), Institut de Génétique et de Biologie Moléculaire et Cellulaire (IGBMC), Université de Strasbourg (UNISTRA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Kazan Federal University (KFU), EMBL Heidelberg, DIAMOND Light source, STFC Rutherford Appleton Laboratory (RAL), Science and Technology Facilities Council (STFC), Architecture et Réactivité de l'ARN (ARN), Institut de biologie moléculaire et cellulaire (IBMC), Université de Strasbourg (UNISTRA)-Centre National de la Recherche Scientifique (CNRS)-Université de Strasbourg (UNISTRA)-Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS), Yusupova, Gulnara, Division of Structural Biology, University of Oxford [Oxford], Institut de génétique et biologie moléculaire et cellulaire (IGBMC), and Université Louis Pasteur - Strasbourg I-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)

Subjects

0301 basic medicine, Peptidyl transferase, Protein Conformation, [SDV.BBM.BS] Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], Science, Potassium, Metal ions in aqueous solution, [SDV]Life Sciences [q-bio], General Physics and Astronomy, chemistry.chemical_element, 02 engineering and technology, Crystallography, X-Ray, Ribosome, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Protein structure, RNA, Transfer, X-Ray Diffraction, Cations, Escherichia coli, Protein biosynthesis, lcsh:Science, ComputingMilieux_MISCELLANEOUS, X-ray crystallography, Multidisciplinary, [SDV.BBM.BS]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], biology, Thermus thermophilus, Cryoelectron Microscopy, RNA, General Chemistry, 021001 nanoscience & nanotechnology, 030104 developmental biology, chemistry, Protein Biosynthesis, Biophysics, biology.protein, lcsh:Q, Crystallization, 0210 nano-technology, Ribosomes, Macromolecule

Abstract

The ribosome, the largest RNA-containing macromolecular machinery in cells, requires metal ions not only to maintain its three-dimensional fold but also to perform protein synthesis. Despite the vast biochemical data regarding the importance of metal ions for efficient protein synthesis and the increasing number of ribosome structures solved by X-ray crystallography or cryo-electron microscopy, the assignment of metal ions within the ribosome remains elusive due to methodological limitations. Here we present extensive experimental data on the potassium composition and environment in two structures of functional ribosome complexes obtained by measurement of the potassium anomalous signal at the K-edge, derived from long-wavelength X-ray diffraction data. We elucidate the role of potassium ions in protein synthesis at the three-dimensional level, most notably, in the environment of the ribosome functional decoding and peptidyl transferase centers. Our data expand the fundamental knowledge of the mechanism of ribosome function and structural integrity., Metal ions play essential roles in myriads of biological processes, from catalytic co-factors to supporting protein and nucleic acid structures. Here the authors use long-wavelength X-ray diffraction to locate hundreds of potassium ions taking part in the formation of rRNA tertiary structure, mediating rRNA–protein interactions and supporting ribosomal protein structures and function.

Published

2019

47. Identifying dynamic, partially occupied residues using anomalous scattering

Author

Vitaliy Mykhaylyk, Christian M. Orr, Armin Wagner, Zhen Yan, Scott Horowitz, S. Rocchio, Kamel El Omari, Ramona Duman, Loïc Salmon, James C.A. Bardwell, University of Michigan [Ann Arbor], University of Michigan System, Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome] (UNIROMA), DIAMOND Light source, STFC Rutherford Appleton Laboratory (RAL), Science and Technology Facilities Council (STFC), Centre de RMN à très hauts champs de Lyon (CRMN), École normale supérieure de Lyon (ENS de Lyon)-Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), Howard Hughes Medical Institute [Chevy Chase] (HHMI), Howard Hughes Medical Institute (HHMI), University of Denver, Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], and École normale supérieure - Lyon (ENS Lyon)-Université Claude Bernard Lyon 1 (UCBL)

Subjects

Models, Molecular, Protein Conformation, [SDV]Life Sciences [q-bio], Crystal structure, Electron, 010402 general chemistry, Kinetic energy, Crystallography, X-Ray, 01 natural sciences, Molecular physics, Crystal, 03 medical and health sciences, Structural Biology, protein folding, chaperones, anomalous scattering, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, crystallography, ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, Physics, 0303 health sciences, Anomalous scattering, [SDV.BBM.BS]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], Protein dynamics, Escherichia coli Proteins, [SDV.BBM.BM]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Molecular biology, Research Papers, 0104 chemical sciences, [SDV.BBM.BP]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biophysics, Kinetics, Beamline, partially occupied residues, protein dynamics, Protein folding, Periplasmic Proteins, Carrier Proteins, Crystallization, Molecular Chaperones

Abstract

Structural studies of partially occupied, heterogeneous protein systems using crystallography are difficult. Here, methods are presented for detecting these states in crystals., Although often presented as taking single ‘snapshots’ of the conformation of a protein, X-ray crystallography provides an averaged structure over time and space within the crystal. The important but difficult task of characterizing structural ensembles in crystals is typically limited to small conformational changes, such as multiple side-chain conformations. A crystallographic method was recently introduced that utilizes residual electron and anomalous density (READ) to characterize structural ensembles encompassing large-scale structural changes. Key to this method is an ability to accurately measure anomalous signals and distinguish them from noise or other anomalous scatterers. This report presents an optimized data-collection and analysis strategy for partially occupied iodine anomalous signals. Using the long-wavelength-optimized beamline I23 at Diamond Light Source, the ability to accurately distinguish the positions of anomalous scatterers with occupancies as low as ∼12% is demonstrated. The number and positions of these anomalous scatterers are consistent with previous biophysical, kinetic and structural data that suggest that the protein Im7 binds to the chaperone Spy in multiple partially occupied conformations. Finally, READ selections demonstrate that re-measured data using the new protocols are consistent with the previously characterized structural ensemble of the chaperone Spy with its client Im7. This study shows that a long-wavelength beamline results in easily validated anomalous signals that are strong enough to be used to detect and characterize highly disordered sections of crystal structures.

Published

2019

48. Structure and Characterization of Crimean-Congo Hemorrhagic Fever Virus GP38

Author

Julius J. Lutwama, Robert W. Cross, Leslie Lobel, Kamel El Omari, Jason S. McLellan, Kartik Chandran, Crystal L. Moyer, Dafna M. Abelson, Akaash K. Mishra, Thomas W. Geisbert, Daniel J. Deer, Armin Wagner, Larry Zeitlin, Ramona Duman, Zachary A. Bornholdt, and John M. Dye

Subjects

Models, Molecular, Antigenicity, Protein Conformation, Immunology, Heterologous, bunyavirus, Antibodies, Viral, Crystallography, X-Ray, Microbiology, 03 medical and health sciences, Mice, Sequence Analysis, Protein, Virology, Animals, Humans, Cloning, Molecular, Spotlight, Pathogen, 030304 developmental biology, Glycoproteins, X-ray crystallography, chemistry.chemical_classification, Mice, Knockout, 0303 health sciences, Nairovirus, biology, 030306 microbiology, Immunogenicity, Structure and Assembly, nairovirus, biology.organism_classification, 3. Good health, Disease Models, Animal, STAT1 Transcription Factor, chemistry, Insect Science, Hemorrhagic Fever Virus, Crimean-Congo, biology.protein, Intercellular Signaling Peptides and Proteins, Female, Hemorrhagic Fever, Crimean, Antibody, Glycoprotein, Crimean Congo hemorrhagic fever virus

Abstract

Crimean-Congo hemorrhagic fever virus (CCHFV) is a priority pathogen that poses a high risk to public health. Due to the high morbidity and mortality rates associated with CCHFV infection, there is an urgent need to develop medical countermeasures for disease prevention and treatment. CCHFV GP38, a secreted glycoprotein of unknown function unique to the Nairoviridae family, was recently shown to be the target of a protective antibody against CCHFV. Here, we present the crystal structure of GP38, which revealed a novel fold with distant homology to another CCHFV glycoprotein that is suggestive of a gene duplication event. We also demonstrate that antibody 13G8 protects STAT1-knockout mice against heterologous CCHFV challenge using a clinical isolate from regions where CCHFV is endemic. Collectively, these data advance our understanding of GP38 structure and antigenicity and should facilitate future studies investigating its function., Crimean-Congo hemorrhagic fever virus (CCHFV) is the causative agent of the most widespread tick-borne viral infection in humans. CCHFV encodes a secreted glycoprotein (GP38) of unknown function that is the target of a protective antibody. Here, we present the crystal structure of GP38 at a resolution of 2.5 Å, which revealed a novel fold primarily consisting of a 3-helix bundle and a β-sandwich. Sequence alignment and homology modeling showed distant homology between GP38 and the ectodomain of Gn (a structural glycoprotein in CCHFV), suggestive of a gene duplication event. Analysis of convalescent-phase sera showed high titers of GP38 antibodies indicating immunogenicity in humans during natural CCHFV infection. The only protective antibody for CCHFV in an adult mouse model reported to date, 13G8, bound GP38 with subnanomolar affinity and protected against heterologous CCHFV challenge in a STAT1-knockout mouse model. Our data strongly suggest that GP38 should be evaluated as a vaccine antigen and that its structure provides a foundation to investigate functions of this protein in the viral life cycle. IMPORTANCE Crimean-Congo hemorrhagic fever virus (CCHFV) is a priority pathogen that poses a high risk to public health. Due to the high morbidity and mortality rates associated with CCHFV infection, there is an urgent need to develop medical countermeasures for disease prevention and treatment. CCHFV GP38, a secreted glycoprotein of unknown function unique to the Nairoviridae family, was recently shown to be the target of a protective antibody against CCHFV. Here, we present the crystal structure of GP38, which revealed a novel fold with distant homology to another CCHFV glycoprotein that is suggestive of a gene duplication event. We also demonstrate that antibody 13G8 protects STAT1-knockout mice against heterologous CCHFV challenge using a clinical isolate from regions where CCHFV is endemic. Collectively, these data advance our understanding of GP38 structure and antigenicity and should facilitate future studies investigating its function.

Published

2019

49. Future Display Technologies for Automotive Application

Author

Armin Wagner-Gentner, Martin Zobl, Stefan Danner, and Stefan Lutz

Subjects

Customer experience, Materials science, business.industry, Systems engineering, Key (cryptography), Automotive industry, business

Abstract

This paper gives an overview about actual and future automotive display concepts, the influence of highly automated driving, key requirements for BMW display experience and interesting future display technologies for new customer experience. An approach to evaluate technologies is described and a derived comparison between requirements for automotive and CE-device displays is shown. Finally current display technologies are rated.

Published

2019

50. Pre-Gibsonian observations on active touch

Author

Armin Wagner

Subjects

History, Received view of theories, Tactual perception, 050105 experimental psychology, 03 medical and health sciences, 0302 clinical medicine, Germany, Humans, 0501 psychology and cognitive sciences, Narrative, Cutaneous sense, General Psychology, Active touch, 05 social sciences, Historical Article, History, 19th Century, History, 20th Century, Object (philosophy), Epistemology, Touch, Aesthetics, Austria, Psychology, Switzerland, 030217 neurology & neurosurgery, Psychophysiology

Abstract

James J. Gibson's (1962) now-classic "Observations on Active Touch" demonstrated the superiority of active over passive touch in object discrimination tasks and thereby exposed the paradigmatic limits of preceding research. Before Gibson, according to the received view, the sense of touch had been treated as a mere receptive channel, ignoring the hand's explorative movements. This article challenges this common narrative by juxtaposing Gibson's article with research published in the German-speaking parts of Europe between the early 19th and mid-20th centuries. The concept of "active touch" did not originate from Gibson's paper alone, nor should earlier appearances of the term be treated simply as exceptional cases. On the contrary, throughout the 19th century, the concept facilitated fundamental theoretical, cross-disciplinary discussions and ultimately evolved into an object of experimental study on its own.

Published

2016