Your search keyword '"Susan M. Lea"' showing total 258 results

1. Delivering a toxic metal to the active site of urease

Author

Yap Shing Nim, Ivan Yu Hang Fong, Justin Deme, Ka Lung Tsang, Joseph Caesar, Steven Johnson, Longson Tsz Hin Pang, Nicholas Man Hon Yuen, Tin Long Chris Ng, Tung Choi, Yakie Yat Hei Wong, Susan M. Lea, and Kam-Bo Wong

Subjects

Multidisciplinary

Abstract

Urease is a nickel (Ni) enzyme that is essential for the colonization of Helicobacter pylori in the human stomach. To solve the problem of delivering the toxic Ni ion to the active site without diffusing into the cytoplasm, cells have evolved metal carrier proteins, or metallochaperones, to deliver the toxic ions to specific protein complexes. Ni delivery requires urease to form an activation complex with the urease accessory proteins UreFD and UreG. Here, we determined the cryo–electron microscopy structures of H. pylori UreFD/urease and Klebsiella pneumoniae UreD/urease complexes at 2.3- and 2.7-angstrom resolutions, respectively. Combining structural, mutagenesis, and biochemical studies, we show that the formation of the activation complex opens a 100-angstrom-long tunnel, where the Ni ion is delivered through UreFD to the active site of urease.

Published

2023

2. Delineation of Functional Subdomains of Huntingtin Protein and Their Interaction with Hap40

Author

Matthew G. Alteen, Justin C. Deme, Claudia P. Alvarez, Peter Loppnau, Ashley Hutchinson, Alma Seitova, Renu Chandrasekaran, Eduardo Silva Ramos, Christopher Secker, Mona Alqazzaz, Erich E. Wanker, Susan M. Lea, Cheryl H. Arrowsmith, and Rachel Harding

Published

2023

3. Expanding the Huntington’s disease research toolbox; validated subdomain protein constructs for biochemical and structural investigation of huntingtin

Author

Matthew G. Alteen, Justin C. Deme, Claudia P. Alvarez, Peter Loppnau, Ashley Hutchinson, Alma Seitova, Renu Chandrasekaran, Eduardo Silva Ramos, Christopher Secker, Mona Alqazzaz, Erich E. Wanker, Susan M. Lea, Cheryl H Arrowsmith, and Rachel J. Harding

Abstract

Huntington’s disease is characterised by CAG expansion in the huntingtin gene above a critical threshold of~35 repeats, resulting in polyglutamine expansion of the huntingtin protein (HTT). The biological role of wildtype HTT and the associated mechanisms of disease pathology caused by expanded HTT remain incompletely understood, in part, due to challenges characterising interactions between HTT and putative binding partners. Here we describe a biochemical toolkit of rationally designed, high-quality recombinant HTT subdomains; one spanning the N-terminal HEAT and bridge domains (NTD) and the second spanning the C-terminal HEAT domain (CTD). Using biophysical methods and cryo-electron microscopy, we show these smaller subdomains are natively folded and can associate to reconstitute a functional full-length HTT structure capable of forming a near native-like complex with 40 kDa HTT-associated protein (HAP40). We report biotin-tagged variants of these subdomains, as well as full-length HTT, that permit immobilisation of each protein for quantitative biophysical assays without impacting protein quality. We demonstrate the CTD alone can form a stable complex when co-expressed with HAP40, which can be structurally resolved. The CTD-HAP40 complex binds the NTD, with a dissociation constant of approximately 10 nM as measured by bio-layer interferometry. We validate the interaction between the CTD and HAP40 using a luciferase two-hybrid assay and use subdomain constructs to demonstrate their respective stabilization of HAP40 in cells. These open-source biochemical tools will enable the wider HD community to study fundamental HTT biology, discover new macromolecular or small-molecule binding partners and map interaction sites across this very large protein.

Published

2022

4. Cryo-EM diversifies

Author

Susan M. Lea and Pamela A. Williams

Subjects

Models, Molecular, Structural Biology, Protein Conformation, Cryoelectron Microscopy, Molecular Biology

Published

2022

5. The DNA transporter ComEC has metal‐dependent nuclease activity that is important for natural transformation

Author

Ben C. Berks, Susan M. Lea, and Augustinas Silale

Subjects

competence, Biological Transport, Active, Bacillus subtilis, natural transformation, Microbiology, 03 medical and health sciences, chemistry.chemical_compound, Bacterial Proteins, Multienzyme Complexes, Extracellular, nuclease, Molecular Biology, Research Articles, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Nuclease, Deoxyribonucleases, DNA transporter, biology, Phosphoric Diester Hydrolases, 030306 microbiology, DNA transport, biology.organism_classification, DNA Transformation Competence, Gram‐positive bacteria, Transformation (genetics), Enzyme, chemistry, Biochemistry, biology.protein, Transformation, Bacterial, CTD, DNA, Research Article

Abstract

In the process of natural transformation bacteria import extracellular DNA molecules for integration into their genome. One strand of the incoming DNA molecule is degraded, whereas the remaining strand is transported across the cytoplasmic membrane. The DNA transport channel is provided by the protein ComEC. Many ComEC proteins have an extracellular C‐terminal domain (CTD) with homology to the metallo‐β‐lactamase fold. Here we show that this CTD binds Mn2+ ions and exhibits Mn2+‐dependent phosphodiesterase and nuclease activities. Inactivation of the enzymatic activity of the CTD severely inhibits natural transformation in Bacillus subtilis. These data suggest that the ComEC CTD is a nuclease responsible for degrading the nontransforming DNA strand during natural transformation and that this process is important for efficient DNA import., During natural transformation in bacteria one DNA strand is transported into the cytoplasm via the membrane protein ComEC while the other strand is degraded. Here we show that the C‐terminal domain of ComEC has a nuclease activity that is important for natural transformation in B. subtilis. Thus, this domain is likely to be responsible for digesting the non‐transforming DNA strand.

Published

2021

6. Structure and mechanism of the proton-driven motor that powers Type 9 secretion and gliding motility

Author

Felicity Alcock, Rory Hennell James, Frederic Lauber, Ben C. Berks, Augustinas Silale, Steven Johnson, Andreas Kjӕr, Justin C. Deme, and Susan M. Lea

Subjects

Microbiology (medical), Gliding motility, Movement, Immunology, Applied Microbiology and Biotechnology, Microbiology, Flavobacterium, Article, 03 medical and health sciences, Bacterial Proteins, Protein Domains, Genetics, Molecular motor, Inner membrane, Secretion, Bacterial Secretion Systems, 030304 developmental biology, 0303 health sciences, ATP synthase, biology, 030306 microbiology, Chemistry, Cryoelectron Microscopy, Cell Biology, Single Molecule Imaging, Transmembrane domain, Structural biology, Periplasm, biology.protein, Biophysics, Protein Multimerization, Protons, Bacterial outer membrane, Porphyromonas gingivalis

Abstract

Three classes of ion-driven protein motors have been identified to date: ATP synthase, the bacterial flagellar motor and a proton-driven motor that powers gliding motility and the type 9 protein secretion system in Bacteroidetes bacteria. Here, we present cryo-electron microscopy structures of the gliding motility/type 9 protein secretion system motors GldLM from Flavobacterium johnsoniae and PorLM from Porphyromonas gingivalis. The motor is an asymmetric inner membrane protein complex in which the single transmembrane helices of two periplasm-spanning GldM/PorM proteins are positioned inside a ring of five GldL/PorL proteins. Mutagenesis and single-molecule tracking identify protonatable amino acid residues in the transmembrane domain of the complex that are important for motor function. Our data provide evidence for a mechanism in which proton flow results in rotation of the periplasm-spanning GldM/PorM dimer inside the intra-membrane GldL/PorL ring to drive processes at the bacterial outer membrane. Using cryo-electron microscopy, the authors describe the structure and function of a molecular motor powering both the Bacteroidetes type 9 protein secretion system and the associated gliding motility apparatus.

Published

2021

7. Symmetry mismatch in the MS-ring of the bacterial flagellar rotor explains structural coordination of secretion and rotation

Author

Emily Furlong, Susan M. Lea, Justin C. Deme, Lucas Kuhlen, Yu Hang Fong, and Steven Johnson

Subjects

Microbiology (medical), Models, Molecular, Stator, Protein Conformation, Immunology, Flagellum, Bacterial physiology, Ring (chemistry), Rotation, Applied Microbiology and Biotechnology, Microbiology, Article, law.invention, 03 medical and health sciences, Structure-Activity Relationship, Protein structure, Bacterial Proteins, law, Electron microscopy, Genetics, Inner membrane, Protein Interaction Domains and Motifs, Bacterial Secretion Systems, 030304 developmental biology, Physics, Spores, Bacterial, Bacterial structural biology, 0303 health sciences, Bacteria, 030306 microbiology, Rotor (electric), Molecular Motor Proteins, Membrane Proteins, Cell Biology, Symmetry (physics), Chemical physics, Flagella, Pathogens, Protein Multimerization

Abstract

The bacterial flagellum is a complex, self-assembling, nanomachine that confers motility to the cell. Despite great variation across species, all flagella are ultimately constructed from a helical propellor attached to a motor embedded in the inner membrane. The motor consists of a series of stator units surrounding a central rotor made up of two ring complexes, the MS-ring and the C-ring. Despite many studies, high resolution structural information is still completely lacking for the MS-ring of the rotor, and proposed mismatches in stoichiometry between the two rings have long provided a source of confusion for the field. We here present structures of the Salmonella MS-ring, revealing an unprecedented level of inter- and intra-chain symmetry variation that provides a structural explanation for the ability of the MS-ring to function as a complex and elegant interface between the two main functions of the flagellum, protein secretion and rotation.

Published

2020

8. The substrate specificity switch FlhB assembles onto the export gate to regulate type three secretion

Author

Joseph J. E. Caesar, Andreas Zeitler, Samuel Wagner, Joseph Fisher, Sandra Bäurle, Lucas Kuhlen, Justin C. Deme, Susan M. Lea, Rebecca Debo, and Steven Johnson

Subjects

0301 basic medicine, Models, Molecular, Science, 030106 microbiology, Protein domain, General Physics and Astronomy, Gating, Flagellum, General Biochemistry, Genetics and Molecular Biology, Article, Protein Structure, Secondary, Substrate Specificity, 03 medical and health sciences, Protein structure, Bacterial Proteins, Protein Domains, Cryoelectron microscopy, Escherichia coli, Secretion, lcsh:Science, Bacterial Secretion Systems, Vibrio, Multidisciplinary, Chemistry, General Chemistry, Periplasmic space, 3. Good health, Transport protein, Transmembrane domain, Protein Transport, 030104 developmental biology, Biophysics, lcsh:Q, Pathogens, Structural biology, Hydrophobic and Hydrophilic Interactions

Abstract

Protein secretion through type-three secretion systems (T3SS) is critical for motility and virulence of many bacteria. Proteins are transported through an export gate containing three proteins (FliPQR in flagella, SctRST in virulence systems). A fourth essential T3SS protein (FlhB/SctU) functions to “switch” secretion substrate specificity once the growing hook/needle reach their determined length. Here, we present the cryo-electron microscopy structure of an export gate containing the switch protein from a Vibrio flagellar system at 3.2 Å resolution. The structure reveals that FlhB/SctU extends the helical export gate with its four predicted transmembrane helices wrapped around FliPQR/SctRST. The unusual topology of the FlhB/SctU helices creates a loop wrapped around the bottom of the closed export gate. Structure-informed mutagenesis suggests that this loop is critical in gating secretion and we propose that a series of conformational changes in the T3SS trigger opening of the gate through interactions between FlhB/SctU and FliPQR/SctRST., Export of proteins by type three secretion systems occurs through an export gate that is localized in the periplasm. Here, the authors present the cryo-EM structure of the Vibrio mimicus export gate complex with FlhB, which plays a major role in switching of the specificity of secretion substrates and propose a mechanism for export gate opening.

Published

2020

9. Structures of the Type IX Secretion/Gliding Motility Motor from across the Phylum

Author

Rory, Hennell James, Justin C, Deme, Alicia, Hunter, Ben C, Berks, and Susan M, Lea

Subjects

Bacterial Proteins, Bacteroidetes, Cryoelectron Microscopy, Adhesins, Bacterial, Bacterial Secretion Systems

Abstract

Gliding motility using cell surface adhesins, and export of proteins by the type IX secretion system (T9SS) are two phylum-specific features of the Bacteroidetes. Both of these processes are energized by the GldLM motor complex, which transduces the proton motive force at the inner membrane into mechanical work at the outer membrane. We previously used cryo-electron microscopy to solve the structure of the GldLM motor core from Flavobacterium johnsoniae at 3.9-Å resolution (R. Hennell James, J. C. Deme, A. Kjaer, F. Alcock, et al., Nat Microbiol 6:221-233, 2021, https://dx.doi.org/10.1038/s41564-020-00823-6). Here, we present structures of homologous complexes from a range of pathogenic and environmental

Published

2022

10. Mechanism of lipid droplet formation by the yeast Sei1/Ldb16 Seipin complex

Author

Phillip J. Stansfeld, Mike F. Renne, Justin C. Deme, Robin A. Corey, Pedro Carvalho, Susan M. Lea, and Yoel A. Klug

Subjects

Models, Molecular, Saccharomyces cerevisiae Proteins, Science, Phospholipid, General Physics and Astronomy, Saccharomyces cerevisiae, Molecular Dynamics Simulation, Endoplasmic Reticulum, General Biochemistry, Genetics and Molecular Biology, Seipin, Article, Mitochondrial Proteins, 03 medical and health sciences, chemistry.chemical_compound, Membrane Lipids, 0302 clinical medicine, Lipid droplet, GTP-Binding Protein gamma Subunits, Organelle, Phospholipids, Triglycerides, 030304 developmental biology, 0303 health sciences, Multidisciplinary, Endoplasmic reticulum, Membrane Proteins, General Chemistry, Lipid Droplets, QP, eye diseases, Transmembrane protein, chemistry, Membrane protein, Biophysics, lipids (amino acids, peptides, and proteins), 030217 neurology & neurosurgery, Biogenesis

Abstract

Lipid droplets (LDs) are universal lipid storage organelles with a core of neutral lipids, such as triacylglycerols, surrounded by a phospholipid monolayer. This unique architecture is generated during LD biogenesis at endoplasmic reticulum (ER) sites marked by Seipin, a conserved membrane protein mutated in lipodystrophy. Here structural, biochemical and molecular dynamics simulation approaches reveal the mechanism of LD formation by the yeast Seipin Sei1 and its membrane partner Ldb16. We show that Sei1 luminal domain assembles a homooligomeric ring, which, in contrast to other Seipins, is unable to concentrate triacylglycerol. Instead, Sei1 positions Ldb16, which concentrates triacylglycerol within the Sei1 ring through critical hydroxyl residues. Triacylglycerol recruitment to the complex is further promoted by Sei1 transmembrane segments, which also control Ldb16 stability. Thus, we propose that LD assembly by the Sei1/Ldb16 complex, and likely other Seipins, requires sequential triacylglycerol-concentrating steps via distinct elements in the ER membrane and lumen., Lipid droplet biogenesis is orchestrated by the conserved membrane protein Seipin via an unknown mechanism. Here, the authors use structural, biochemical and molecular dynamics simulation approaches to reveal the mechanism of lipid droplet formation by the yeast Seipin Sei1 and its partner Ldb16.

Published

2022

11. Structures of the Type IX Secretion/gliding motility motor from across the phylum Bacteroidetes

Author

Rory Hennell James, Justin C. Deme, Alicia Hunter, Ben C. Berks, and Susan M. Lea

Subjects

animal structures, Virology, Microbiology

Abstract

Gliding motility using cell surface adhesins and export of proteins by the Type IX Secretion System (T9SS) are two phylum-specific features of the Bacteroidetes. Both of these processes are energized by the GldLM motor complex which transduces the protonmotive force at the inner membrane into mechanical work at the outer membrane. We previously used cryo-electron microscopy to solve the structure of the GldLM motor core from Flavobacterium johnsoniae at 3.9 Å resolution (Nat Microbiol (2021) 6: 221-233). Here we present structures of homologous complexes from a range of pathogenic and environmental Bacteroidetes species at up to 3.0 Å resolution. These structures show that the architecture of the GldLM motor core is conserved across the Bacteroidetes phylum although there are species-specific differences at the N-terminus of GldL. The resolution improvements reveal a cage-like structure that ties together the membrane-proximal cytoplasmic region of GldL and influences gliding function. These findings add detail to our structural understanding of bacterial ion-driven motors that drive the T9SS and gliding motility.ImportanceMany bacteria in the Bacteroidetes phylum use the Type IX Secretion System to secrete proteins across their outer membrane. Most of these bacteria can also glide across surfaces using adhesin proteins that are propelled across the cell surface. Both secretion and gliding motility are driven by the GldLM protein complex which forms a nanoscale electrochemical motor. We used cryo-electron microscopy to study the structure of the GldLM protein complex from different species including the human pathogens Porphyromonas gingivalis and Capnocytophaga canimorsus. The organisation of the motor is conserved across species, but we find species-specific structural differences and resolve motor features at higher resolution. This work improves our understanding of the Type IX Secretion System, which is a virulence determinant in human and animal diseases.

Published

2022

12. Structure and function of a family of tick-derived complement inhibitors targeting properdin

Author

Katharina Braunger, Jiyoon Ahn, Matthijs M. Jore, Steven Johnson, Terence T. L. Tang, Dennis V. Pedersen, Gregers R. Andersen, and Susan M. Lea

Subjects

Science, Immunology, Complement Pathway, Alternative, Complement, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], General Physics and Astronomy, chemical and pharmacologic phenomena, urologic and male genital diseases, General Biochemistry, Genetics and Molecular Biology, Article, Arthropod Proteins, All institutes and research themes of the Radboud University Medical Center, Rhipicephalus, Animals, Humans, Amino Acid Sequence, Complement Activation, X-ray crystallography, Multidisciplinary, Properdin, General Chemistry, Complement C3, female genital diseases and pregnancy complications, Kinetics, Complement Inactivating Agents, Sequence Alignment

Abstract

Activation of the serum-resident complement system begins a cascade that leads to activation of membrane-resident complement receptors on immune cells, thus coordinating serum and cellular immune responses. Whilst many molecules act to control inappropriate activation, Properdin is the only known positive regulator of the human complement system. By stabilising the alternative pathway C3 convertase it promotes complement self-amplification and persistent activation boosting the magnitude of the serum complement response by all triggers. In this work, we identify a family of tick-derived alternative pathway complement inhibitors, hereafter termed CirpA. Functional and structural characterisation reveals that members of the CirpA family directly bind to properdin, inhibiting its ability to promote complement activation, and leading to potent inhibition of the complement response in a species specific manner. We provide a full functional and structural characterisation of a properdin inhibitor, opening avenues for future therapeutic approaches., Properdin is the only known positive regulator of the human complement system, stabilising the convertase C3 in the alternative pathway of complement activation. Here, the authors report the identification and characterisation of a species-specific properdin inhibitor CirpA, derived from tick saliva.

Published

2022

13. Structural basis of antifolate recognition and transport by PCFT

Author

Susan M. Lea, J Huo, I D Goldman, Justin C. Deme, Philip C. Biggin, Simon Newstead, Gabriel Kuteyi, Joanne L. Parker, Raymond J. Owens, and Zhemeng Wu

Subjects

Models, Molecular, 0301 basic medicine, Brush border, Pemetrexed, 01 natural sciences, Article, 03 medical and health sciences, Methylating Agent, chemistry.chemical_compound, Immune system, 0103 physical sciences, Humans, chemistry.chemical_classification, Multidisciplinary, Cellular metabolism, 010304 chemical physics, Cryoelectron Microscopy, Biological Transport, Transporter, Amino acid, 030104 developmental biology, chemistry, Biochemistry, Antifolate, Nucleic acid, Folic Acid Antagonists, Protons, Apoproteins, Proton-Coupled Folate Transporter

Abstract

Folates (also known as vitamin B9) have a critical role in cellular metabolism as the starting point in the synthesis of nucleic acids, amino acids and the universal methylating agent S-adenylsmethionine(1,2). Folate deficiency is associated with a number of developmental, immune and neurological disorders(3–5). Mammals cannot synthesize folates de novo; several systems have therefore evolved to take up folates from the diet and distribute them within the body(3,6). The proton-coupled folate transporter (PCFT) (also known as SLC46A1) mediates folate uptake across the intestinal brush border membrane and the choroid plexus(4,7), and is an important route for the delivery of antifolate drugs in cancer chemotherapy(8–10). How PCFT recognizes folates or antifolate agents is currently unclear. Here we present cryo-electron microscopy structures of PCFT in a substrate-free state and in complex with a new-generation antifolate drug (pemetrexed). Our results provide a structural basis for understanding antifolate recognition and provide insights into the pH-regulated mechanism of folate transport mediated by PCFT.

Published

2021

14. Molecular basis for redox control by the human cystine/glutamate antiporter System xc

Author

Gabriel Kuteyi, Simon Newstead, Justin C. Deme, Dimitrios Kolokouris, Joanne L. Parker, Philip C. Biggin, and Susan M. Lea

Subjects

chemistry.chemical_classification, 0303 health sciences, Reactive oxygen species, 010304 chemical physics, Antiporter, Allosteric regulation, Cystine, Glutathione, Ligand (biochemistry), 01 natural sciences, 3. Good health, 03 medical and health sciences, chemistry.chemical_compound, chemistry, Biochemistry, 0103 physical sciences, Intracellular, 030304 developmental biology, Cysteine

Abstract

Cysteine plays an essential role in cellular redox homeostasis as a key constituent of the tripeptide glutathione (GSH). A rate limiting step in cellular GSH synthesis is the availability of cysteine. However, circulating cysteine exists in the blood as the oxidised di-peptide cystine, requiring specialised transport systems for its import into the cell. System xc- is a dedicated cystine transporter, importing cystine in exchange for intracellular glutamate. To counteract elevated levels of reactive oxygen species in cancerous cells system xc- is frequently upregulated, making it an attractive target for anticancer therapies. However, the molecular basis for ligand recognition remains elusive, hampering efforts to specifically target this transport system. Here we present the cryo-EM structure of system xc- in both the apo and glutamate bound states. Structural comparisons reveal an allosteric mechanism for ligand discrimination, supported by molecular dynamics and cell-based assays, establishing a mechanism for cystine transport in human cells.

Published

2021

15. The conserved C2 phospholipid‐binding domain in Delta contributes to robust Notch signalling

Author

Richard Suckling, Torcato Martins, Yao Meng, Boguslawa Korona, Steven Johnson, Susan M. Lea, Penny A. Handford, Sarah J. Bray, Martins, Torcato [0000-0002-9359-7111], Handford, Penny A [0000-0002-0590-7651], Lea, Susan M [0000-0001-9287-8053], Bray, Sarah J [0000-0002-1642-599X], and Apollo - University of Cambridge Repository

Subjects

Notch ligands, Phospholipid, Notch signaling pathway, Endogeny, Development, EMBO40, Ligands, Biochemistry, Article, chemistry.chemical_compound, EMBO37, Structural Biology, Genetics, Drosophila Proteins, Humans, Molecular Biology, Phospholipids, C2 domain, phospholipid, Receptors, Notch, Membrane Proteins, Articles, Phenotype, EMBO11, Cell biology, C2 Domains, chemistry, Delta, Phospholipid Binding, Notch binding, Drosophila, Function (biology), Signal Transduction

Abstract

Accurate Notch signalling is critical for development and homeostasis. Fine‐tuning of Notch–ligand interactions has substantial impact on signalling outputs. Recent structural studies have identified a conserved N‐terminal C2 domain in human Notch ligands which confers phospholipid binding in vitro. Here, we show that Drosophila ligands Delta and Serrate adopt the same C2 domain structure with analogous variations in the loop regions, including the so‐called β1‐2 loop that is involved in phospholipid binding. Mutations in the β1‐2 loop of the Delta C2 domain retain Notch binding but have impaired ability to interact with phospholipids in vitro. To investigate its role in vivo, we deleted five residues within the β1‐2 loop of endogenous Delta. Strikingly, this change compromises ligand function. The modified Delta enhances phenotypes produced by Delta loss‐of‐function alleles and suppresses that of Notch alleles. As the modified protein is present on the cell surface in normal amounts, these results argue that C2 domain phospholipid binding is necessary for robust signalling in vivo fine‐tuning the balance of trans and cis ligand–receptor interactions., Engineered mutations in the conserved N‐terminal C2 domains of endogenous Delta and Serrate show that perturbing one of the protruding loops conferring phospholipid binding leads to defective Notch signalling in vivo, confirming its contribution to normal ligand activity.

Published

2021

16. Molecular basis for redox control by the human cystine/glutamate antiporter system xc

Author

Joanne L. Parker, Justin C. Deme, Dimitrios Kolokouris, Gabriel Kuteyi, Philip C. Biggin, Susan M. Lea, and Simon Newstead

Subjects

Amino Acid Transport System y+, Fusion Regulatory Protein 1, Heavy Chain, Science, General Physics and Astronomy, Glutamic Acid, 01 natural sciences, Biochemistry, General Biochemistry, Genetics and Molecular Biology, Antiporters, Article, 03 medical and health sciences, Neoplasms, 0103 physical sciences, Humans, Cysteine, 030304 developmental biology, Cancer, 0303 health sciences, Multidisciplinary, 010304 chemical physics, Cryoelectron Microscopy, General Chemistry, Glutathione, 3. Good health, Up-Regulation, HEK293 Cells, Cystine, Reactive Oxygen Species, Oxidation-Reduction

Abstract

Cysteine plays an essential role in cellular redox homoeostasis as a key constituent of the tripeptide glutathione (GSH). A rate limiting step in cellular GSH synthesis is the availability of cysteine. However, circulating cysteine exists in the blood as the oxidised di-peptide cystine, requiring specialised transport systems for its import into the cell. System xc− is a dedicated cystine transporter, importing cystine in exchange for intracellular glutamate. To counteract elevated levels of reactive oxygen species in cancerous cells system xc− is frequently upregulated, making it an attractive target for anticancer therapies. However, the molecular basis for ligand recognition remains elusive, hampering efforts to specifically target this transport system. Here we present the cryo-EM structure of system xc− in both the apo and glutamate bound states. Structural comparisons reveal an allosteric mechanism for ligand discrimination, supported by molecular dynamics and cell-based assays, establishing a mechanism for cystine transport in human cells., System xc- is a cystine transporter that is expressed in the plasma membrane and imports cystine in exchange for intracellular glutamate. Here, the authors present the cryo-EM structure of human system xc- both in the apo form and the glutamate bound state, and further supported by molecular dynamics and cell-based assays they discuss its cystine transport mechanism.

Published

2021

17. Cryo-EM structure of PepT2 reveals structural basis for proton-coupled peptide and prodrug transport in mammals

Author

Joanne L. Parker, Simon Newstead, Justin C. Deme, Philip C. Biggin, Zhiyi Wu, Raymond J. Owens, Jiandong Huo, Susan M. Lea, and Gabriel Kuteyi

Subjects

Cryo-electron microscopy, Biophysics, Peptide, Peptide binding, Peptide Transporter 1, Molecular dynamics, Structural Biology, Animals, Prodrugs, Research Articles, chemistry.chemical_classification, Mammals, Multidisciplinary, Symporters, Cryoelectron Microscopy, Substrate (chemistry), food and beverages, SciAdv r-articles, Membrane Transport Proteins, Transporter, Prodrug, Ligand (biochemistry), Rats, chemistry, Biochemistry, Protons, Peptides, Research Article

Abstract

Structure of PepT2 reveals binding model for peptide recognition and enables a more rationalized approach to prodrug design., The SLC15 family of proton-coupled solute carriers PepT1 and PepT2 play a central role in human physiology as the principal route for acquiring and retaining dietary nitrogen. A remarkable feature of the SLC15 family is their extreme substrate promiscuity, which has enabled the targeting of these transporters for the improvement of oral bioavailability for several prodrug molecules. Although recent structural and biochemical studies on bacterial homologs have identified conserved sites of proton and peptide binding, the mechanism of peptide capture and ligand promiscuity remains unclear for mammalian family members. Here, we present the cryo–electron microscopy structure of the outward open conformation of the rat peptide transporter PepT2 in complex with an inhibitory nanobody. Our structure, combined with molecular dynamics simulations and biochemical and cell-based assays, establishes a framework for understanding peptide and prodrug recognition within this pharmaceutically important transporter family.

Published

2021

18. Molecular structure of the intact bacterial flagellar basal body

Author

Joseph J. E. Caesar, Ashley L. Nord, Justin C. Deme, Emily Furlong, Fabienne F. V. Chevance, Susan M. Lea, Kelly T. Hughes, Richard M. Berry, Steven Johnson, Sir William Dunn School of Pathology [Oxford], University of Oxford [Oxford], Center for Structural Biology (CCR, NCI), Central Oxford Structural Molecular Imaging Centre, University of Oxford, Centre de Biochimie Structurale [Montpellier] (CBS), Centre National de la Recherche Scientifique (CNRS)-Université de Montpellier (UM)-Institut National de la Santé et de la Recherche Médicale (INSERM), University of Utah, Department of Biology, University of Oxford, Department of Physics, University of Oxford, Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Montpellier (UM)-Centre National de la Recherche Scientifique (CNRS), and Nord, Ashley

Subjects

Microbiology (medical), [SDV.BBM.BS] Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], Immunology, Flagellum, Rotation, Applied Microbiology and Biotechnology, Microbiology, Article, law.invention, Cell wall, 03 medical and health sciences, Bacterial Proteins, Salmonella, law, Genetics, Inner membrane, ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, 0303 health sciences, [SDV.BBM.BS]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], 030306 microbiology, Chemistry, Cryoelectron Microscopy, Cell Biology, Basal Bodies, Molecular machine, Membrane, Flagella, Bushing, Drive shaft, Biophysics, Bacterial outer membrane

Abstract

The bacterial flagellum is a macromolecular protein complex that enables motility in many species. Bacterial flagella self-assemble a strong, multicomponent drive shaft that couples rotation in the inner membrane to the micrometre-long flagellar filament that powers bacterial swimming in viscous fluids1–3. Here, we present structures of the intact Salmonella flagellar basal body4, encompassing the inner membrane rotor, drive shaft and outer-membrane bushing, solved using cryo-electron microscopy to resolutions of 2.2–3.7 A. The structures reveal molecular details of how 173 protein molecules of 13 different types assemble into a complex spanning two membranes and a cell wall. The helical drive shaft at one end is intricately interwoven with the rotor component with both the export gate complex and the proximal rod forming interactions with the MS-ring. At the other end, the drive shaft distal rod passes through the LP-ring bushing complex, which functions as a molecular bearing anchored in the outer membrane through interactions with the lipopolysaccharide. The in situ structure of a protein complex capping the drive shaft provides molecular insights into the assembly process of this molecular machine. The in situ cryo-electron microscopy structure of the intact Salmonella flagellar basal body—including the inner membrane rotor, drive shaft and outer membrane bushing complex—elucidates the mechanisms of assembly of this complex macromolecular structure that enables bacterial motility.

Published

2021

19. Molecular Basis for Bordetella pertussis Interference with Complement, Coagulation, Fibrinolytic, and Contact Activation Systems: the Cryo-EM Structure of the Vag8-C1 Inhibitor Complex

Author

Arun Dhillon, Dorina Roem, Susan M. Lea, Emily Furlong, Ilse Jongerius, Justin C. Deme, Steven D. Johnson, Landsteiner Laboratory, Paediatric Infectious Diseases / Rheumatology / Immunology, and AII - Inflammatory diseases

Subjects

Models, Molecular, Bordetella pertussis, Proteases, Type V Secretion Systems, Plasma protein binding, Serpin, Microbiology, single-particle cryo-EM, C1-inhibitor, 03 medical and health sciences, Bacterial Proteins, Protein Domains, Virology, Virulence Factors, Bordetella, Blood Coagulation, Reactive center, complement system, autotransporters, immune evasion, 030304 developmental biology, 0303 health sciences, Binding Sites, Virulence, biology, 030306 microbiology, Chemistry, Fibrinolysis, Cryoelectron Microscopy, serpin, Complement System Proteins, respiratory system, bacterial infections and mycoses, biology.organism_classification, QR1-502, bacterial pathogenicity, three-dimensional structure, respiratory tract diseases, 3. Good health, Complement system, Cell biology, Mutation, biology.protein, Autotransporter domain, C1-INH, Complement C1 Inhibitor Protein, Research Article, Protein Binding

Abstract

The structure of a 10-kDa protein complex is one of the smallest to be determined using cryo-electron microscopy at high resolution. The structure reveals that C1-INH is sequestered in an inactivated state by burial of the reactive center loop in Vag8., Complement, contact activation, coagulation, and fibrinolysis are serum protein cascades that need strict regulation to maintain human health. Serum glycoprotein, a C1 inhibitor (C1-INH), is a key regulator (inhibitor) of serine proteases of all the above-mentioned pathways. Recently, an autotransporter protein, virulence-associated gene 8 (Vag8), produced by the whooping cough pathogen, Bordetella pertussis, was shown to bind to C1-INH and interfere with its function. Here, we present the structure of the Vag8–C1-INH complex determined using cryo-electron microscopy at a 3.6-Å resolution. The structure shows a unique mechanism of C1-INH inhibition not employed by other pathogens, where Vag8 sequesters the reactive center loop of C1-INH, preventing its interaction with the target proteases.

Published

2021

20. Cryo-EM structure and resistance landscape of M. tuberculosis MmpL3: An emergent therapeutic target

Author

Philip W. Fowler, Simon Newstead, Joanne L. Parker, Susan M. Lea, Oliver Adams, Justin C. Deme, and Consortium, CRyPTIC

Subjects

Tuberculosis, Resistance (ecology), Cryoelectron Microscopy, Membrane Transport Proteins, Drug resistance, Computational biology, Disease, Biology, medicine.disease, biology.organism_classification, Mycobacterium tuberculosis, Lipid transporter, Bacterial Proteins, Structural Biology, Drug Resistance, Bacterial, Mutation, medicine, Drug Binding Site, Molecular Biology, Infectious agent

Abstract

Tuberculosis (TB) is the leading cause of death from a single infectious agent and in 2019 an estimated 10 million people worldwide contracted the disease. Although treatments for TB exist, continual emergence of drug-resistant variants necessitates urgent development of novel antituberculars. An important new target is the lipid transporter MmpL3, which is required for construction of the unique cell envelope that shields Mycobacterium tuberculosis (Mtb) from the immune system. However, a structural understanding of the mutations in Mtb MmpL3 that confer resistance to the many preclinical leads is lacking, hampering efforts to circumvent resistance mechanisms. Here, we present the cryoelectron microscopy structure of Mtb MmpL3 and use it to comprehensively analyze the mutational landscape of drug resistance. Our data provide a rational explanation for resistance variants local to the central drug binding site, and also highlight a potential alternative route to resistance operating within the periplasmic domain.

Published

2021

21. Targeting properdin - Structure and function of a novel family of tick-derived complement inhibitors

Author

Terence Tang, Susan M. Lea, Gregers R. Andersen, Ahn J, Braunger K, Steven D. Johnson, Pedersen Dv, and Matthijs M. Jore

Subjects

Immune system, Chemistry, Regulator, Alternative complement pathway, Properdin, Complement receptor, C3-convertase, Complement (complexity), Cell biology, Complement system

Abstract

Activation of the serum-resident complement system begins a cascade that leads to activation of membrane-resident complement receptors on immune cells, thus coordinating serum and cellular immune responses. Whilst many molecules act to control inappropriate activation, Properdin is the only known positive regulator of the human complement system. By stabilising the alternative pathway C3 convertase it promotes complement self-amplification and persistent activation boosting the magnitude of the serum complement response by all triggers.We have identified a novel family of alternative pathway complement inhibitors, hereafter termed CirpA. Functional and structural characterisation reveals that CirpA family directly bind to properdin, inhibiting its ability to promote complement activation, and leading to potent inhibition of the complement response in a species specific manner.For the first time this study provides a full functional and structural characterization of a properdin inhibitor, opening avenues for future therapeutic approaches.

Published

2021

22. HAP40 orchestrates huntingtin structure for differential interaction with polyglutamine expanded exon 1

Author

Matthieu Schapira, Alexander Lemak, Alma Seitova, Justin C. Deme, Peter Loppnau, Cheryl H. Arrowsmith, Ashley Hutchinson, Sem Tamara, Rachel Harding, Albert J. R. Heck, Susan M. Lea, Jeffrey P. Cantle, Xiaobing Zuo, Magdalena M. Szewczyk, Johannes F. Hevler, Jeffrey B. Carroll, and Lixin Fan

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Huntingtin, Architecture domain, Drug discovery, Chemistry, Mutant, Wild type, Polyglutamine tract, nervous system diseases, Cell biology, Exon, nervous system, mental disorders, Gene

Abstract

Huntington’s disease results from expansion of a glutamine-coding CAG tract in the huntingtin (HTT) gene, producing an aberrantly functioning form of HTT. Both wildtype and disease-state HTT form a hetero-dimer with HAP40 of unknown functional relevance. We demonstrate in vivo that HTT and HAP40 cellular abundance are coupled. Integrating data from a 2.6 Å cryo-electron microscopy structure, cross-linking mass spectrometry, small-angle X-ray scattering, and modeling, we provide a near-atomic-level view of HTT, its molecular interaction surfaces and compacted domain architecture, orchestrated by HAP40. Native mass-spectrometry reveals a remarkably stable hetero-dimer, potentially explaining the cellular inter-dependence of HTT and HAP40. The polyglutamine tract containing N-terminal exon 1 region of HTT is dynamic, but shows greater conformational variety in the mutant than wildtype exon 1. By providing novel insight into the structural consequences of HTT polyglutamine expansion, our data provide a foundation for future functional and drug discovery studies targeting Huntington’s disease.

Published

2021

23. SIMPLE 3.0. Stream single-particle cryo-EM analysis in real time

Author

Steven Johnson, Joseph J. E. Caesar, Chiara Machello, Susan M. Lea, Molly L. Tang, Simon Kiesewetter, Justin C. Deme, Dominika Elmlund, Hans Elmlund, and Cyril F. Reboul

Subjects

Data processing, Workstation, Computer science, business.industry, Real-time computing, Stream image processing, Single-particle, Image processing, Article, law.invention, Data flow diagram, Data acquisition, lcsh:Biology (General), Structural Biology, law, Cluster analysis, business, lcsh:QH301-705.5, Execution model, Real-time, Graphical user interface, ComputingMethodologies_COMPUTERGRAPHICS, Cryo-EM

Abstract

Graphical abstract, We here introduce the third major release of the SIMPLE (Single-particle IMage Processing Linux Engine) open-source software package for analysis of cryogenic transmission electron microscopy (cryo-EM) movies of single-particles (Single-Particle Analysis, SPA). Development of SIMPLE 3.0 has been focused on real-time data processing using minimal CPU computing resources to allow easy and cost-efficient scaling of processing as data rates escalate. Our stream SPA tool implements the steps of anisotropic motion correction and CTF estimation, rapid template-based particle identification and 2D clustering with automatic class rejection. SIMPLE 3.0 additionally features an easy-to-use web-based graphical user interface (GUI) that can be run on any device (workstation, laptop, tablet or phone) and supports a remote multi-user environment over the network. The new project-based execution model automatically records the executed workflow and represents it as a flow diagram in the GUI. This facilitates meta-data handling and greatly simplifies usage. Using SIMPLE 3.0, it is possible to automatically obtain a clean SP data set amenable to high-resolution 3D reconstruction directly upon completion of the data acquisition, without the need for extensive image processing post collection. Only minimal standard CPU computing resources are required to keep up with a rate of ∼300 Gatan K3 direct electron detector movies per hour. SIMPLE 3.0 is available for download from simplecryoem.com.

Published

2020

24. Molecular basis forB. pertussisinterference with complement, coagulation, fibrinolytic and contact activation systems: The cryo-EM structure of the Vag8-C1 inhibitor complex

Author

Dorina Roem, Steven Johnson, Arun Dhillon, Emily Furlong, Susan M. Lea, Ilse Jongerius, and Justin C. Deme

Subjects

chemistry.chemical_classification, Bordetella pertussis, Proteases, biology, Virulence, biology.organism_classification, C1-inhibitor, Cell biology, Serine, chemistry, Coagulation, biology.protein, Autotransporter domain, Glycoprotein

Abstract

Complement, contact activation, coagulation, and fibrinolysis are serum protein cascades that need strict regulation to maintain human health. Serum glycoprotein, C1-inhibitor (C1-INH) is a key regulator (inhibitor) of serine proteases of all the above-mentioned pathways. Recently, an autotransporter protein, Virulence Associated Gene 8 (Vag8) produced by the whopping cough causing pathogen,Bordetella pertussishas been shown to bind and interfere with C1-INH function. Here we present the structure of Vag8: C1-INH complex determined using cryo-electron microscopy at 3.6 Å resolution. The structure shows a unique mechanism of C1-INH inhibition not employed by other pathogens where Vag8 sequesters the Reactive Centre Loop of the C1-INH preventing its interaction with the target proteases.ImportanceThe structure 105 kDa protein complex is one of the smallest to be determined using cryo-electron microscopy at high resolution. The mechanism of disrupting C1-INH revealed by the structure is crucial to understand how pathogens by producing a single virulence factor can disturb several homeostasis pathways. Virulence mechanisms such as the one described here assume more importance given the emerging evidence about dysregulation of contact activation, coagulation and fibrinolysis leading to COVID-19 pneumonia.

Published

2020

25. Decision letter: The flagellar motor of Vibrio alginolyticus undergoes major structural remodeling during rotational switching

Author

Edward H. Egelman, Susan M. Lea, and Chi Aizawa

Subjects

Vibrio alginolyticus, biology, Chemistry, biology.organism_classification, Structural remodeling, Cell biology

Published

2020

26. WITHDRAWN: SIMPLE 3.0. Stream single-particle cryo-EM analysis in real time

Author

Steven Johnson, Simon Kiesewetter, Susan M. Lea, Hans Elmlund, Justin C. Deme, Cyril F. Reboul, Dominika Elmlund, Chiara Machello, Joseph J. E. Caesar, and Molly L. Tang

Subjects

0303 health sciences, 03 medical and health sciences, 0302 clinical medicine, Structural Biology, Cryo-electron microscopy, Simple (abstract algebra), Computer science, Particle, 030217 neurology & neurosurgery, 030304 developmental biology, Computational physics

Published

2020

27. The role of toxin:antitoxin systems and insertion sequences in the loss of virulence in Shigella sonnei

Author

Gareth McVicker, Susan M. Lea, Christoph M. Tang, Sarah Hollingshead, Mariya Lobanovska, Jessica E. Martyn, Kristoffer Skovbo Winther, and Giulia Pilla

Subjects

Shigella flexneri, Plasmid, biology, vapBC, medicine, Virulence, Shigella sonnei, Shigella, Antitoxin, biology.organism_classification, medicine.disease_cause, Pathogenicity island, Microbiology

Abstract

SUMMARYThe Shigella plasmid, pINV, contains a 30 kb pathogenicity island (PAI) encoding a Type III secretion system (T3SS) which is essential for virulence. During growth in the laboratory, avirulent colonies of Shigella (which do not express a T3SS) arise spontaneously. Avirulence in Shigella flexneri mostly follows loss of the PAI, following recombination between insertion sequences (ISs) on pINV; toxin:antitoxin (TA) systems on pINV promote its retention through post-segregational killing (PSK). We show that avirulence in Shigella sonnei mainly results from plasmid loss, consistent with previous findings; IS-mediated PAI deletions can occur in S. sonnei, but through different ISs than in S. flexneri. We investigated the molecular basis for frequent loss of the S. sonnei plasmid, pINVSsonn. Introduction into pINVSsonn of CcdAB and GmvAT, toxin:antitoxin TA systems in pINV from S. flexneri but not S. sonnei, reduced plasmid loss and the emergence of avirulent bacteria. However, plasmid loss remained the leading cause of avirulence. We show that a single amino acid difference in the VapC toxin of the VapBC TA system in pINV also contributes to high frequency plasmid loss in S. sonnei compared to S. flexneri. Our findings demonstrate that the repertoire of ISs, complement of TA systems, and polymorphisms in TA systems influence plasmid dynamics and virulence loss in S. sonnei. Understanding the impact of polymorphisms should be informative about how TA systems contribute to PSK, and could be exploited for generating strains with stable plasmids.

Published

2020

28. Structure of a proton-powered molecular motor that drives protein transport and gliding motility

Author

R Hennell James, Ben C. Berks, Felicity Alcock, Augustinas Silale, Andreas Kjaer, Frederic Lauber, Justin C. Deme, and Susan M. Lea

Subjects

Transmembrane domain, ATP synthase, biology, Gliding motility, Molecular motor, biology.protein, Biophysics, Inner membrane, Bacterial outer membrane, Bacterial cell structure, Transport protein

Abstract

SummaryIon-driven motors are rare in biology. The archetypes of the three classes identified to date are ATP synthase, the bacterial flagellar motor, and a proton-driven motor that powers gliding motility and protein secretion in Bacteroidetes bacteria. Whilst the molecular mechanism of ATP synthase is now well understood, structural information is lacking for the other two classes of motor. Here we present the structure of the Bacteroidetes gliding motility motor determined by cryo-electron microscopy. The motor is an asymmetric inner membrane protein complex in which the single transmembrane helices of two periplasm-spanning GldM proteins are positioned within a ring of five GldL proteins. Combining mutagenesis and single-molecule tracking, we identify protonatable amino acid residues within the transmembrane domain of the complex that are important for motor function. Our data imply a mechanism in which proton flow leads the periplasm-spanning GldM dimer to rotate with respect to the intra-membrane GldL ring to drive processes at the bacterial outer membrane. This work provides a molecular basis for understanding how the gliding motility motor is able to transduce the energy of the inner membrane protonmotive force across the bacterial cell envelope.

Published

2020

29. Structures of the stator complex that drives rotation of the bacterial flagellum

Author

Justin C. Deme, Holly Monkhouse, Samuel Johnson, A Muellbauer, R Hennell James, James W. Coulton, Owen N. Vickery, Ben C. Berks, Phillip J. Stansfeld, Susan M. Lea, and Thomas Griffiths

Subjects

Microbiology (medical), Rotation, Stator, Protein subunit, Immunology, Bacillus subtilis, Flagellum, Applied Microbiology and Biotechnology, Microbiology, 01 natural sciences, Article, law.invention, 03 medical and health sciences, Bacterial Proteins, law, 0103 physical sciences, Genetics, Torque, 030304 developmental biology, Clostridium, Physics, 0303 health sciences, biology, 010304 chemical physics, 030306 microbiology, Rotor (electric), Molecular Motor Proteins, Propeller, Cell Biology, biology.organism_classification, QR, Mechanism (engineering), Flagella, Biophysics, Vibrio mimicus

Abstract

SummaryThe bacterial flagellum is the proto-typical protein nanomachine and comprises a rotating helical propeller attached to a membrane-embedded motor complex1. The motor consists of a central rotor surround by stator units that couple ion flow across the cytoplasmic membrane to torque generation. Here we present the structures of stator complexes from multiple bacterial species, allowing interpretation of the extensive body of data on stator mechanism. The structures reveal an unexpected asymmetric A5B2 subunit assembly in which the five A subunits enclose the two B subunits. Comparison to novel structures of other ion-driven motors indicates that this A5B2 architecture is fundamental to bacterial systems that couple energy from ion-flow to generate mechanical work at a distance, and suggests that such events involve rotation in the motor structures.

Published

2020

30. FHR-1 Binds to C-Reactive Protein and Enhances Rather than Inhibits Complement Activation

Author

T. Sakari Jokiranta, Ádám I. Csincsi, Mihály Józsi, Joseph J. E. Caesar, Agustín Tortajada, Barbara Uzonyi, Éva Kárpáti, Zsóka Szabó, Marcell Cserhalmi, Susan M. Lea, Zoltán Prohászka, Zsófia Bánlaki, and Santiago Rodríguez de Córdoba

Subjects

0301 basic medicine, Immunology, Complement C3-C5 Convertases, Biology, Ligands, Macular Degeneration, 03 medical and health sciences, 0302 clinical medicine, Complement C3b Inactivator Proteins, Human Umbilical Vein Endothelial Cells, Humans, Immunology and Allergy, Complement Activation, Binding Sites, Complement component 2, CD46, Extracellular Matrix, Complement system, Serum Amyloid P-Component, C-Reactive Protein, 030104 developmental biology, Biochemistry, Complement Factor H, Factor H, Complement C3b, embryonic structures, Alternative complement pathway, biology.protein, CFHR5, Protein Binding, 030215 immunology, Complement control protein

Abstract

Factor H–related protein (FHR) 1 is one of the five human FHRs that share sequence and structural homology with the alternative pathway complement inhibitor FH. Genetic studies on disease associations and functional analyses indicate that FHR-1 enhances complement activation by competitive inhibition of FH binding to some surfaces and immune proteins. We have recently shown that FHR-1 binds to pentraxin 3. In this study, our aim was to investigate whether FHR-1 binds to another pentraxin, C-reactive protein (CRP), analyze the functional relevance of this interaction, and study the role of FHR-1 in complement activation and regulation. FHR-1 did not bind to native, pentameric CRP, but it bound strongly to monomeric CRP via its C-terminal domains. FHR-1 at high concentration competed with FH for CRP binding, indicating possible complement deregulation also on this ligand. FHR-1 did not inhibit regulation of solid-phase C3 convertase by FH and did not inhibit terminal complement complex formation induced by zymosan. On the contrary, by binding C3b, FHR-1 allowed C3 convertase formation and thereby enhanced complement activation. FHR-1/CRP interactions increased complement activation via the classical and alternative pathways on surfaces such as the extracellular matrix and necrotic cells. Altogether, these results identify CRP as a ligand for FHR-1 and suggest that FHR-1 enhances, rather than inhibits, complement activation, which may explain the protective effect of FHR-1 deficiency in age-related macular degeneration.

Published

2017

31. An inhibitor of complement C5 provides structural insights into activation

Author

Martin P. Reichhardt, Steven Johnson, Terence Tang, Thomas Morgan, Nchimunya Tebeka, Niko Popitsch, Justin C. Deme, Matthijs M. Jore, and Susan M. Lea

Subjects

0301 basic medicine, complement regulation, Male, Erythrocytes, Guinea Pigs, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Crystallography, X-Ray, Biochemistry, Hemolysis, single-particle cryo-EM, Arthropod Proteins, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, 0302 clinical medicine, Protein Domains, Rhipicephalus, Animals, Humans, Saliva, innate immunity, Complement Activation, X-ray crystallography, Multidisciplinary, Sheep, Cryoelectron Microscopy, Complement C5, Feeding Behavior, Biological Sciences, Immunity, Innate, 3. Good health, Rats, inhibitor, 030104 developmental biology, PNAS Plus, 030220 oncology & carcinogenesis, Female, Rabbits, Protein Binding

Abstract

Significance The complement system is a crucial antimicrobial system in the human body. However, controlling its regulation is essential, and failure to do so is implicated in a number of clinical inflammatory pathologies leading to great interest in therapeutic complement inhibition. We have identified and characterized a class of complement inhibitors from biting ticks. Utilizing both cryoelectron microscopy and X-ray crystallography we provide a comprehensive understanding of their mechanism of inhibition at the level of the terminal pathway of complement. We present a high-resolution cryoelectron microscopy structure of complement C5, the molecule targeted by the major therapeutic Eculizumab. In addition, we reveal the fold of the CirpT family of tick inhibitors and their unique mode of inhibition., The complement system is a crucial part of innate immune defenses against invading pathogens. The blood-meal of the tick Rhipicephalus pulchellus lasts for days, and the tick must therefore rely on inhibitors to counter complement activation. We have identified a class of inhibitors from tick saliva, the CirpT family, and generated detailed structural data revealing their mechanism of action. We show direct binding of a CirpT to complement C5 and have determined the structure of the C5–CirpT complex by cryoelectron microscopy. This reveals an interaction with the peripheral macro globulin domain 4 (C5_MG4) of C5. To achieve higher resolution detail, the structure of the C5_MG4–CirpT complex was solved by X-ray crystallography (at 2.7 Å). We thus present the fold of the CirpT protein family, and provide detailed mechanistic insights into its inhibitory function. Analysis of the binding interface reveals a mechanism of C5 inhibition, and provides information to expand our biological understanding of the activation of C5, and thus the terminal complement pathway.

Published

2020

32. Structure of a Proton-Powered Motor that Drives Protein Transport and Gliding Motility

Author

Andreas Kjaer, Justin C. Deme, Felicity Alcock, Frederic Lauber, Susan M. Lea, Rory Hennell-James, Ben C. Berks, Steven Johnson, and Augustinas Silale

Subjects

Transmembrane domain, Secretory protein, ATP synthase, biology, Chemistry, Gliding motility, Membrane protein complex, biology.protein, Biophysics, Inner membrane, Bacterial outer membrane, Transport protein

Abstract

Ion-driven motors are amongst the most fascinating protein nanomachines known. The archetypes of the three classes identified to date are ATP synthase, the bacterial flagellar motor, and a proton-driven motor that powers gliding motility and protein secretion in Bacteroidetes bacteria. Here we present the structure of the Bacteroidetes gliding motility motor. The motor is an asymmetric inner membrane protein complex in which the single transmembrane helices of two periplasm-spanning GldM proteins are positioned within a ring of five GldL proteins. Combining mutagenesis and single-molecule tracking, we identify protonatable amino acid residues within the transmembrane domain of the complex that are important for motor function. Our data imply a mechanism in which proton flow leads the periplasm-spanning GldM dimer to rotate with respect to the intra-membrane GldL ring to drive processes at the bacterial outer membrane.

Published

2020

33. Evaluating CBT Clinical Competence with Standardised Role Plays and Patient Therapy Sessions

Author

David M. Clark, Sarah Beale, Sheena Liness, Susan M. Lea, Colette R. Hirsch, and Suzanne Byrne

Subjects

Predictive validity, 050103 clinical psychology, medicine.medical_specialty, medicine.medical_treatment, education, Experimental and Cognitive Psychology, 03 medical and health sciences, IAPT, 0302 clinical medicine, Competence, medicine, 0501 psychology and cognitive sciences, Competence (human resources), Weak relationship, Standardised role play, 05 social sciences, 030227 psychiatry, Clinical Psychology, Inter-rater reliability, Convergent validity, Assessment methods, Physical therapy, Cognitive therapy, Patient recordings, Clinical competence, Psychology, Cognitive behaviour therapy (CBT)

Abstract

Standardised role-plays (SR) have been proposed as an alternative to recordings of patients’ therapy sessions (PTS) to assess therapist competence during CBT training. This study compared the following properties of SR assessments with established PTS assessments: interrater reliability, responsiveness to training, convergent validity of competence ratings, and predictive validity for academic outcomes. SR and PTS were both rated using the Cognitive Therapy Scale Revised (CTS-R) to assess CBT trainees’ (n = 88) level of competence at the beginning and end of training, and at one-year follow-up. Both methods demonstrated excellent inter-rater reliability between pairs of course tutors (ICC range = .81–.93) and good reliability between tutors and an external assessor (ICC range = .71–.74). CTS-R scores for both SR and PTS increased across training to reach the competence threshold and remained stable at follow-up. However, there was only a weak relationship between the two assessment methods. Further refinement of SR as a CBT assessment method is indicated.

Published

2019

34. Core components of bacterial protein secretion systems revealed at high resolution by cryo-electron microscopy

Author

Susan M. Lea, Steven L. Johnson, Lucas Kuhlen, Patrizia Abrusci, Justin C. Deme, Ben C. Berks, and Frederic Lauber

Subjects

Inorganic Chemistry, Bacterial protein, Structural Biology, Cryo-electron microscopy, Chemistry, Core component, Biophysics, High resolution, General Materials Science, Secretion, Physical and Theoretical Chemistry, Condensed Matter Physics, Biochemistry

Published

2019

35. Structure of the bacterial flagellar rotor MS-ring: a minimum inventory/maximum diversity system

Author

Steven Johnson, Yu Hang Fong, Emily Furlong, Susan M. Lea, Justin C. Deme, and Lucas Kuhlen

Subjects

Physics, 0303 health sciences, Rotor (electric), Stator, Structure (category theory), Flagellum, Ring (chemistry), Rotation, Symmetry (physics), law.invention, 03 medical and health sciences, 0302 clinical medicine, law, Inner membrane, Biological system, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

The bacterial flagellum is a complex, self-assembling, nanomachine that confers motility on the cell. Despite great variation across species, all flagella are ultimately constructed from a helical propellor attached to a motor embedded in the inner membrane. The motor consists of a series of stator units surrounding a central rotor made up of two ring complexes, the MS-ring and the C-ring. Despite many studies, high resolution structural information is still completely lacking for the MS-ring of the rotor, and proposed mismatches in stoichiometry between the two rings have long provided a source of confusion for the field. We here present structures of the Salmonella MS-ring, revealing an unprecedented level of inter- and intra-chain symmetry variation that provides a structural explanation for the ability of the MS-ring to function as a complex and elegant interface between the two main functions of the flagellum, protein secretion and rotation.

Published

2019

36. Structural control for the coordinated assembly into functional pathogenic type-3 secretion systems

Author

Frank DiMaio, Oliver Vesper, Sean Miletic, Nikolaus Goessweiner-Mohr, Samuel Wagner, Susan M. Lea, Thomas C. Marlovits, Lucas Kuhlen, Jiri Wald, Julia Mayr, Matthias J. Brunner, Vadim Kotov, and Wolfgang Lugmayr

Subjects

Protein filament, Docking (molecular), Cryo-electron microscopy, Effector, Chemistry, Biophysics, Basal body, Secretion, Molecular machine, Type three secretion system

Abstract

Functional injectisomes of the type-3 secretion system assemble into highly defined and stoichiometric bacterial molecular machines essential for infecting human and other eukaryotic cells. However, the mechanism that governs the regulated step-wise assembly process from the nucleation-phase, to ring-assembly, and the filamentous phase into a membrane embedded needle complex is unclear. We here report that the formation of a megadalton-sized needle complexes fromSalmonella entericaserovar Typhimurium (SPI-1,Salmonellapathogenicity island-1) with proper stoichiometries is highly structurally controlled competing against the self-assembly propensity of injectisome components, leading to a highly unusual structurally-pleiotropic phenotype. The structure of the entire needle complex from pathogenic injectisomes was solved by cryo electron microscopy, focused refinements (2.5-4 Å) and co-variation analysis revealing an overall asymmetric arrangement containing cyclic, helical, and asymmetric sub-structures. The centrally located export apparatus assembles into a conical, pseudo-helical structure and provides a structural template that guides the formation of a 24-mer cyclic, surrounding ring, which then serves as a docking interface comprising three different conformations for sixteen N-terminal InvG subunits of the outer secretin ring. Unexpectedly, the secretin ring excludes the 16thprotein chain at the C-terminal outer ring, resulting in a pleiotropic 16/15-mer ring and consequently to an overall 24:16/15 basal body structure. Finally, we report how the transition from the pseudo-helical export apparatus into the helical filament is structurally resolved to generate the protein secretion channel, which provides the structural basis to restrict access of unfolded effector substrates. These results highlight the diverse molecular signatures required for a highly coordinated assembly process and provide the molecular basis for understanding triggering and transport of unfolded proteins through injectisomes.

Published

2019

37. The structure of SALSA/DMBT1 SRCR domains reveal the conserved ligand-binding mechanism of the ancient SRCR-fold

Author

Martin Parnov Reichhardt, Vuokko Loimaranta, Steven Johnson, and Susan M. Lea

Subjects

chemistry.chemical_classification, 0303 health sciences, 03 medical and health sciences, Cation binding, 0302 clinical medicine, Chemistry, SUPERFAMILY, Computational biology, Scavenger receptor, Ligand (biochemistry), 030304 developmental biology, 030215 immunology, Amino acid

Abstract

The scavenger receptor cysteine-rich (SRCR) family of proteins comprise more than 20 membrane-associated and secreted molecules. Characterised by the presence of one or more copies of the ~110 amino acid SRCR domain, this class of proteins have widespread functions as anti-microbial molecules, scavenger- and signalling-receptors. Despite the high level of structural conservation of SRCR domains, no molecular basis for ligand interaction has been described. The SRCR protein SALSA, also known as dmbt1/gp340, is a key player in mucosal immunology. Based on detailed structures of the SALSA SRCR domains 1 and 8, we here reveal a novel universal ligand binding mechanism for SALSA ligands. The binding interface incorporates a dual cation binding site, which is highly conserved across the SRCR super family. Along with the well-described cation dependency on most SRCR domain-ligand interactions, our data suggest that the binding mechanism described for the SALSA SRCR domains is applicable to all SRCR domains. We thus propose to have identified in SALSA a conserved functional mechanism for ligand recognition by the SRCR class of proteins.

Published

2019

38. The flagellar substrate specificity switch protein FlhB assembles onto the extra-membrane export gate to regulate type three secretion

Author

Justin C. Deme, Rebecca Debo, Susan M. Lea, Steven Johnson, Samuel Wagner, Andreas Zeitler, Sandra Bäurle, Joseph Fisher, and Lucas Kuhlen

Subjects

0303 health sciences, 030306 microbiology, Chemistry, Mutagenesis, Virulence, Gating, Type three secretion system, 03 medical and health sciences, Transmembrane domain, Membrane, Membrane protein, Biophysics, Secretion, 030304 developmental biology

Abstract

Export of proteins through type three secretion systems (T3SS) is critical for motility and virulence of many major bacterial pathogens. Proteins are transported through an export gate complex consisting of three proteins (FliPQR in flagellar systems, SctRST in virulence systems) that were initially annotated as membrane proteins, but which we have recently shown assemble into an extra-membranous helical assembly. A fourth putative membrane protein (FlhB/SctU) is essential to the export process, and also functions to “switch” secretion substrate specificity once the growing hook/needle structures reach their determined length. Here we present the structure of an export gate containing the switch protein from a Vibrio polar flagellar system at 3.2 Å resolution by cryo-electron microscopy. The structure reveals that the FlhB/SctU further extends the helical export gate assembly with its four putative transmembrane helices adopting an out-of-membrane location, wrapped around the other export gate components at the base of the structure. The unusual topology of the switch protein helices creates a loop that wraps around the bottom of the closed export gate complex. Structure-informed mutagenesis suggests that this loop is critical in gating secretion and we propose that a series of conformational changes in the type 3 secretion system trigger opening of the export gate through the interactions between FlhB/SctU and FliPQR/SctRST.

Published

2019

39. A novel inhibitor of complement C5 provides structural insights into activation

Author

Thomas Morgan, Nchimunya Tebka, Niko Popitsch, Justin C. Deme, Steven Johnson, Terence Tang, Susan M. Lea, Martin Parnov Reichhardt, and Matthijs M. Jore

Subjects

Complement component 5, 0303 health sciences, Innate immune system, Protein family, Chemistry, 030302 biochemistry & molecular biology, Computational biology, Complement system, 03 medical and health sciences, Rhipicephalus pulchellus, Mechanism of action, Direct binding, medicine, medicine.symptom, Function (biology), 030304 developmental biology

Abstract

The complement system is a crucial part of innate immune defences against invading pathogens. The blood-meal of the tick Rhipicephalus pulchellus lasts for days, and the tick must therefore rely on inhibitors to counter complement activation. We have identified a novel class of inhibitors from tick saliva, the CirpT family, and generated detailed structural data revealing their mechanism of action. We show direct binding of a CirpT to complement C5 and have determined the structure of the C5-CirpT complex by cryo-electron microscopy. This reveals an interaction with the peripheral macro globulin domain 4 (C5_MG4) of C5. To achieve higher resolution detail, the structure of the C5_MG4-CirpT complex was solved by X-ray crystallography (at 2.7 Å). We thus present the novel fold of the CirpT protein family, and provide detailed mechanistic insights into its inhibitory function. Analysis of the binding interface reveals a novel mechanism of C5 inhibition, and provides information to expand our biological understanding of the activation of C5, and thus the terminal complement pathway.

Published

2019

40. Structural insights into a novel properdin-binding tick inhibitor from Rhipicephalus pulchellus

Author

Jiyoon Ahn, Steven Johnson, and Susan M. Lea

Subjects

0301 basic medicine, 03 medical and health sciences, Rhipicephalus pulchellus, 030104 developmental biology, Immunology, Properdin, Complement Inhibitors, Biology, Tick, biology.organism_classification, Molecular Biology, Microbiology

Published

2019

41. Multi-professional IAPT CBT training: clinical competence and patient outcomes

Author

Sarah Beale, Susan M. Lea, David M. Clark, Suzanne Byrne, Colette R. Hirsch, and Sheena Liness

Subjects

Adult, Male, medicine.medical_treatment, competence, education, clinical outcome, Anxiety, IAPT, Multi professional, medicine, Humans, Longitudinal Studies, Competence (human resources), Medical education, Depressive Disorder, Cognitive Behavioral Therapy, Depression, Improving Access to Psychological Therapies, General Medicine, anxiety, Mental health, Anxiety Disorders, Cognitive behavioral therapy, Clinical Psychology, Treatment Outcome, CBT training, depression, Workforce, Female, Clinical Competence, Clinical competence, medicine.symptom, Psychology

Abstract

Background:There is international interest in the training of psychological therapists to deliver evidence-based treatment for common mental health problems. The UK Improving Access to Psychological Therapies (IAPT) programme, one of the largest training initiatives, relies on competent therapists to successfully deliver cognitive behaviour therapy (CBT) and promote good patient outcome.Aims:To evaluate an IAPT CBT training course by assessing if trainees’ clinical skills improve during training and reach competency standards, and to report patient outcome for submitted training cases. To investigate a possible relationship between trainee competence and patient outcome. To explore professional differences during training.Method:CBT trainee (n = 252) competence was assessed via audio recordings of therapy sessions at the beginning, middle and end of training. Patient pre- to post-treatment outcomes were extracted from submitted training cases (n = 1927). Differences in professional background were examined across competence, academic final grade and tutorial support.Results:CBT trainees attained competence by the end of the course with 77% (anxiety recordings) and 72% (depression recordings) improving reliably. Training cases reported pre- to post-treatment effect sizes of 1.08–2.26 across disorders. CBT competence predicted a small variance in clinical outcome for depression cases. Differences in professional background emerged, with clinical psychologists demonstrating greater competence and higher academic grades. Trainees without a core professional background required more additional support to achieve competence.Conclusions:Part of a new CBT therapist workforce was successfully trained to deliver relatively brief treatment effectively. Trainees without a core profession can be successfully trained to competence, but may need additional support. This has implications for workforce training.

Published

2019

42. The structure of an injectisome export gate demonstrates conservation of architecture in the core export gate between flagellar and virulence type three secretion systems

Author

Justin C. Deme, Susan M. Lea, Patrizia Abrusci, Lucas Kuhlen, and Steven Johnson

Subjects

0303 health sciences, 03 medical and health sciences, Membrane protein, 030306 microbiology, Chemistry, Virulence, Secretion, 030304 developmental biology, Cell biology

Abstract

Export of proteins through type three secretion systems (T3SS) is critical for motility and virulence of many major bacterial pathogens. Proteins are exported though a genetically defined export gate complex consisting of three proteins. We have recently shown at 4.2 Å that the flagellar complex of these three putative membrane proteins (FliPQR in flagellar systems, SctRST in virulence systems) assemble into an extra-membrane helical assembly that likely seeds correct assembly of the rod above. Here we present the structure of an equivalent complex from the more fragile Shigella virulence system at 3.5 Å by cryo-electron microscopy. This higher resolution structure reveals further detail and confirms the prediction of structural conservation in this core complex. Analysis of particle heterogeneity also reveals details of how the SctS/FliQ subunits sequentially assemble in the complex.

Published

2019

43. Nonameric structures of the cytoplasmic domain of FlhA and SctV in the context of the full-length protein

Author

Justin C. Deme, Steven L. Johnson, Jerry Y. Cao, Lucas Kuhlen, and Susan M. Lea

Subjects

Models, Molecular, Protein Conformation, Membrane Protein Complexes, Cell Membranes, Secretion Systems, Protomer, Pathology and Laboratory Medicine, Biochemistry, Microbial Physiology, Medicine and Health Sciences, Macromolecular Structure Analysis, Type III Secretion Systems, Electron Microscopy, Bacterial Physiology, Microscopy, 0303 health sciences, Crystallography, Multidisciplinary, Chemistry, Physics, Condensed Matter Physics, Protein Transport, Cell Processes, Flagella, Physical Sciences, Crystal Structure, Medicine, Vibrio parahaemolyticus, Pathogens, Cellular Structures and Organelles, Research Article, Protein Structure, Virulence Factors, Science, Protein subunit, Green Fluorescent Proteins, Context (language use), Flagellum, Research and Analysis Methods, Microbiology, 03 medical and health sciences, Bacterial Proteins, Escherichia coli, Solid State Physics, Inner membrane, Integral Membrane Proteins, Secretion, Molecular Biology, Yersinia enterocolitica, 030304 developmental biology, 030306 microbiology, Cryoelectron Microscopy, Biology and Life Sciences, Membrane Proteins, Proteins, Protein Complexes, Protein Secretion, Bacteriology, Electron Cryo-Microscopy, Cell Biology, Secretory protein, Microscopy, Fluorescence, Membrane protein, Cytoplasm, Biophysics

Abstract

Type three secretion is the mechanism of protein secretion found in bacterial flagella and injectisomes. At its centre is the export apparatus (EA), a complex of five membrane proteins through which secretion substrates pass the inner membrane. While the complex formed by four of the EA proteins has been well characterised structurally, little is known about the structure of the membrane domain of the largest subunit, FlhA in flagella, SctV in injectisomes. Furthermore, the biologically relevant nonameric assembly of FlhA/SctV has been infrequently observed and differences in conformation of the cytoplasmic portion of FlhA/SctV between open and closed states have been suggested to reflect secretion system specific differences. FlhA has been shown to bind to chaperone-substrate complexes in an open state, but in previous assembled ring structures, SctV is in a closed state. Here, we identify FlhA and SctV homologues that can be recombinantly produced in the oligomeric state and study them using cryo-electron microscopy. The structures of the cytoplasmic domains from both FlhA and SctV are in the open state and we observe a conserved interaction between a short stretch of residues at the N-terminus of the cytoplasmic domain, known as FlhAL/SctVL, with a groove on the adjacent protomer’s cytoplasmic domain, which stabilises the nonameric ring assembly.

Published

2021

44. Structure of the Yeast Seipin Reveals Determinants for Lipid Droplet Biogenesis

Author

Yoel A. Klug, Justin C. Deme, Pedro Carvalho, and Susan M. Lea

Subjects

Chemistry, Lipid droplet, Biophysics, Yeast, Biogenesis, Seipin, Cell biology

Published

2021

45. What IAPT CBT High-Intensity Trainees Do After Training

Author

David M. Clark, Susan M. Lea, Sheena Liness, Hannah Parker, and Steffen Nestler

Subjects

Adult, Male, 050103 clinical psychology, medicine.medical_specialty, medicine.medical_treatment, Psychological intervention, Personnel Turnover, CBT, Nice, behavioral disciplines and activities, Health Services Accessibility, 03 medical and health sciences, 0302 clinical medicine, Surveys and Questionnaires, Outcome Assessment, Health Care, follow-up, medicine, Humans, 0501 psychology and cognitive sciences, 030212 general & internal medicine, Cognitive behaviour, CBT supervision, computer.programming_language, Response rate (survey), Career Choice, Cognitive Behavioral Therapy, High intensity, 05 social sciences, Improving Access to Psychological Therapies, General Medicine, Middle Aged, United Kingdom, Psychotherapy, Clinical Psychology, CBT training, Family medicine, Workforce, Cognitive therapy, Anxiety, Female, medicine.symptom, Psychology, computer, Follow-Up Studies

Abstract

Background:The UK Department of Health Improving Access to Psychological Therapies (IAPT) initiative set out to train a large number of therapists in cognitive behaviour therapies (CBT) for depression and anxiety disorders. Little is currently known about the retention of IAPT CBT trainees, or the use of CBT skills acquired on the course in the workplace after training has finished.Aims:This study set out to conduct a follow-up survey of past CBT trainees on the IAPT High Intensity CBT Course at the Institute of Psychiatry, Psychology and Neuroscience (IoPPN), King's College London (KCL), one of the largest IAPT High Intensity courses in the UK.Method:Past trainees (n= 212) across 6 cohorts (2008-2014 intakes) were contacted and invited to participate in a follow-up survey. A response rate of 92.5% (n= 196) was achieved.Results:The vast majority of IAPT trainees continue to work in IAPT services posttraining (79%) and to practise CBT as their main therapy modality (94%); 61% have become CBT supervisors. A minority (23%) have progressed to other senior roles in the services. Shortcomings are reported in the use of out-of-office CBT interventions, the use of disorder-specific outcome measures and therapy recordings to inform therapy and supervision.Conclusions:Past trainees stay working in IAPT services and continue to use CBT methods taught on the course. Some NICE recommended treatment procedures that are likely to facilitate patients’ recovery are not being routinely implemented across IAPT services. The results have implications for the continued roll out of the IAPT programme, and other future large scale training initiatives.

Published

2016

46. Author Correction: Structures of the stator complex that drives rotation of the bacterial flagellum

Author

Steven Johnson, Amy Aron, James W. Coulton, Thomas Griffiths, Susan M. Lea, Owen N. Vickery, Phillip J. Stansfeld, Ben C. Berks, Justin C. Deme, Holly Monkhouse, and Rory Hennell James

Subjects

Microbiology (medical), Physics, Stator, law, Immunology, Genetics, Geometry, Cell Biology, Flagellum, Rotation, Applied Microbiology and Biotechnology, Microbiology, law.invention

Published

2020

47. Structures of SALSA/DMBT1 SRCR domains reveal the conserved ligand-binding mechanism of the ancient SRCR fold

Author

Vuokko Loimaranta, Steven Johnson, Martin Parnov Reichhardt, and Susan M. Lea

Subjects

0301 basic medicine, Health, Toxicology and Mutagenesis, Receptors, Cell Surface, Plant Science, Computational biology, Ligands, Biochemistry, Genetics and Molecular Biology (miscellaneous), 03 medical and health sciences, Protein Domains, Humans, Amino Acid Sequence, Cysteine, Scavenger receptor, Research Articles, Receptors, Scavenger, Binding Sites, 030102 biochemistry & molecular biology, Ecology, Chemistry, Mechanism (biology), Tumor Suppressor Proteins, Calcium-Binding Proteins, SUPERFAMILY, Ligand (biochemistry), DNA-Binding Proteins, 030104 developmental biology, Protein Binding, Research Article

Abstract

The structures of SALSA SRCR domains 1 and 8 reveal a cation-dependent mechanism for ligand recognition, contributing to important roles in the immune system and cellular signalling. The cation-binding sites are conserved across all SRCR domains, suggesting conserved functional mechanisms., The scavenger receptor cysteine-rich (SRCR) family of proteins comprises more than 20 membrane-associated and secreted molecules. Characterised by the presence of one or more copies of the ∼110 amino-acid SRCR domain, this class of proteins have widespread functions as antimicrobial molecules, scavenger receptors, and signalling receptors. Despite the high level of structural conservation of SRCR domains, no unifying mechanism for ligand interaction has been described. The SRCR protein SALSA, also known as DMBT1/gp340, is a key player in mucosal immunology. Based on detailed structural data of SALSA SRCR domains 1 and 8, we here reveal a novel universal ligand-binding mechanism for SALSA ligands. The binding interface incorporates a dual cation-binding site, which is highly conserved across the SRCR superfamily. Along with the well-described cation dependency on most SRCR domain–ligand interactions, our data suggest that the binding mechanism described for the SALSA SRCR domains is applicable to all SRCR domains. We thus propose to have identified in SALSA a conserved functional mechanism for the SRCR class of proteins.

Published

2020

48. The sustained effects of CBT training on therapist competence and patient outcomes

Author

Suzanne Byrne, David M. Clark, Sheena Liness, Colette R. Hirsch, Susan M. Lea, and Sarah Beale

Subjects

050103 clinical psychology, medicine.medical_specialty, Follow-up, medicine.medical_treatment, 05 social sciences, education, Cognitive behavioural therapy (CBT), Psychological therapy, Supervision, Experimental and Cognitive Psychology, Cognitive behaviour therapy, 030227 psychiatry, IAPT, 03 medical and health sciences, Clinical Psychology, 0302 clinical medicine, Competence, Patient outcomes, Cognitive therapy, medicine, Physical therapy, 0501 psychology and cognitive sciences, Psychology, Competence (human resources), Quality of Life Research

Abstract

The continued effectiveness of in-service psychological therapy training requires evaluation. This study assessed therapist competence and patient clinical outcome during cognitive behaviour therapy training and 12+ months post-training. Trainee competence was assessed using audio-recorded sessions rated on the Cognitive Therapy Scale Revised at the beginning (nthinspace=thinspace33) and end of training (nthinspace=thinspace45), and at least 12 months post-training (nthinspace=thinspace45). Pre-to-posttreatment clinical outcome for trainees' patients during the course (nthinspace=thinspace360) and post-training (nthinspace=thinspace360) was evaluated using standardised self-report measures. The relationship between therapist competence and patient outcomes was explored. Trainees achieved competence during training (100%, nthinspace=thinspace45) and largely maintained competence post-training (84%, nthinspace=thinspace38). Patients demonstrated pre-to-posttreatment effect sizes between 1.38 and 1.89 and reliable improvement exceeding 80% during and after training. Competence was not significantly associated with patient outcome. Trainees predominantly maintained competence and achieved good clinical outcomes post-training. Structured training and continued use of regular supervision possibly supported retention of competence.

Published

2018

49. 'It Gave Me My Life Back'

Author

Lynne Callaghan and Susan M. Lea

Subjects

Adult, Male, Domestic Violence, Sociology and Political Science, Community organization, Poison control, Patient Advocacy, Community integration, Patient advocacy, Suicide prevention, Gender Studies, Nursing, Statutory law, Humans, Medicine, 0505 law, Service (business), business.industry, 05 social sciences, Psychosocial Support Systems, United Kingdom, Models, Organizational, Spouse Abuse, 050501 criminology, Domestic violence, Female, business, Community Integration, Law, Social Welfare

Abstract

Community-based advocacy services are important in enabling victims to escape domestic abuse and rebuild their lives. This study evaluated a domestic abuse service. Two phases of research were conducted following case-file analysis ( n = 86): surveys ( n = 22) and interviews ( n = 12) with victims, and interviews with key individuals ( n = 12) based in related statutory and community organizations. The findings revealed the holistic model of legal, practical, mental health–related, and advocacy components resulted in a range of benefits to victims and enhanced interagency partnership working. Core elements of a successful needs-led, victim-centered service could be distilled.

Published

2015

50. Factor H–Related Protein 5 Interacts with Pentraxin 3 and the Extracellular Matrix and Modulates Complement Activation

Author

Miklós Zöldi, Mihály Józsi, Zsófia Bánlaki, Matthew C. Pickering, Kenji Daigo, Anne Kopp, Susan M. Lea, Takao Hamakubo, Joseph J. E. Caesar, Elena Goicoechea de Jorge, Ádám I. Csincsi, Barbara Uzonyi, and Mario Hebecker

Subjects

CHRONIC KIDNEY-DISEASE, CFHR1, Immunology, Biology, Ligands, Complement inhibitor, GLOMERULONEPHRITIS, GLOMERULAR IMMUNE DEPOSITS, BINDING, Humans, Immunology and Allergy, Complement Activation, PTX3, Science & Technology, IDENTIFICATION, Pentraxins, Complement component 2, Complement System Proteins, Recombinant Proteins, C3-convertase, Extracellular Matrix, Complement system, Serum Amyloid P-Component, C-Reactive Protein, C-REACTIVE-PROTEIN, Biochemistry, Factor H, Molecular and Structural Immunology, biology.protein, Alternative complement pathway, HEMOLYTIC-UREMIC SYNDROME, AUTOANTIBODIES, Life Sciences & Biomedicine, CFHR5, Protein Binding

Abstract

The physiological roles of the factor H (FH)-related proteins are controversial and poorly understood. Based on genetic studies, FH-related protein 5 (CFHR5) is implicated in glomerular diseases, such as atypical hemolytic uremic syndrome, dense deposit disease, and CFHR5 nephropathy. CFHR5 was also identified in glomerular immune deposits at the protein level. For CFHR5, weak complement regulatory activity and competition for C3b binding with the plasma complement inhibitor FH have been reported, but its function remains elusive. In this study, we identify pentraxin 3 (PTX3) as a novel ligand of CFHR5. Binding of native CFHR5 to PTX3 was detected in human plasma and the interaction was characterized using recombinant proteins. The binding of PTX3 to CFHR5 is of ∼2-fold higher affinity compared with that of FH. CFHR5 dose-dependently inhibited FH binding to PTX3 and also to the monomeric, denatured form of the short pentraxin C–reactive protein. Binding of PTX3 to CFHR5 resulted in increased C1q binding. Additionally, CFHR5 bound to extracellular matrix in vitro in a dose-dependent manner and competed with FH for binding. Altogether, CFHR5 reduced FH binding and its cofactor activity on pentraxins and the extracellular matrix, while at the same time allowed for enhanced C1q binding. Furthermore, CFHR5 allowed formation of the alternative pathway C3 convertase and supported complement activation. Thus, CFHR5 may locally enhance complement activation via interference with the complement-inhibiting function of FH, by enhancement of C1q binding, and by activating complement, thereby contributing to glomerular disease.

Published

2015