Your search keyword '"Timmins PA"' showing total 57 results

1. Effects of ligand binding on the association properties and conformation in solution of retinoic acid receptors RXR and RAR.

Author

Egea, PF, Egea, PF, Rochel, N, Birck, C, Vachette, P, Timmins, PA, Moras, D, Egea, PF, Egea, PF, Rochel, N, Birck, C, Vachette, P, Timmins, PA, and Moras, D

Abstract

In higher eukaryotes, vitamin A derived metabolites such as 9-cis and all-trans retinoic acid (RA), are involved in the regulation of several essential physiological processes. Their pleiotropic physiological effects are mediated through direct binding to cognate nuclear receptors RXRs and RARs that act as regulated transcription factors belonging to the superfamily of nuclear hormone receptors. Hormone binding to the structurally conserved ligand-binding domain (LBD) of these receptors triggers a conformational change that principally affects the conserved C-terminal transactivation helix H12 involved in transcriptional activation. We report an extensive biophysical solution study of RAR alpha, RXR alpha LBDs and their corresponding RXR alpha/RAR alpha LBD heterodimers combining analytical ultracentrifugation (AUC), small-angle X-ray and neutron scattering (SAXS and SANS) and ab initio three-dimensional shape reconstruction at low resolution. We show that the crystal structures of RXRs and RARs LBDs correlate well with the average conformations observed in solution. Furthermore we demonstrate the effects of 9-cisRA and all-transRA binding on the association properties and conformations of RXR alpha and RAR alpha LBDs in solution. The present study shows that in solution RAR alpha LBD behaves as a monomer in both unliganded and liganded forms. It confirms the existence in solution of a ligand-induced conformational change towards a more compact form of the LBD. It also confirms the stability of the predicted RXR alpha/RAR alpha LBD heterodimers in solution. SAS measurements performed on three different types of RXR alpha/RAR alpha LBD heterodimers (apo/apo, apo/holo and holo/holo) with respect to their ligand-binding site occupancy show the existence of three conformational states depending on the progressive binding of RA stereoisomers on RAR alpha and RXR alpha LBD subunits in the heterodimeric context. These results suggest that the subunits are structurally inde

Published

2001

2. STRUCTURE AND RNA-CONTENT OF THE PROSOMES

Author

COUX, O, NOTHWANG, HG, SCHERRER, K, BERGSMASCHUTTER, W, ARNBERG, AC, TIMMINS, PA, LANGOWSKI, J, COHENADDAD, C, Stratingh Institute of Chemistry, and Groningen Biomolecular Sciences and Biotechnology

Subjects

PROTEASE COMPLEX, PROSOME, MULTICATALYTIC PROTEINASE, ORGANIZATION, RIBONUCLEOPROTEIN, UBIQUITIN, ELECTRON MICROSCOPY, MULTICATALYTIC PROTEINASE COMPLEX, MOLECULAR-WEIGHT, IDENTITY, LIGHT SCATTERING, PROTEASOME, NEUTRON SCATTERING, IMAGE-ANALYSIS, PARTICLE, CRYO-ELECTRON MICROSCOPY

Abstract

Duck erythroblasts prosomes were analysed by small angle neutron scattering (SANS), dynamic light scattering and (cryo-)electron microscopy. A molecular weight of approximately 720,000 +/- 50,000, a radius of gyration of 64 +/- 2 angstrom and a hydrodynamic radius of approximately 86 angstrom were obtained. Electron micrographs show a hollow cylinder-like particle with a diameter of 120 angstrom, a height of 170 angstrom and a diameter of 40 angstrom for the cavity, built of four discs, the two outer ones being more pronounced than those in the center. Results from SANS indicate less then 5% of RNA in the purified prosomes, but nuclease protection assays confirm its presence.

Published

1992

3. Detergent structure in tetragonal crystals of OmpF porin

Author

Pebay-Peyroula, E, primary, Garavito, RM, additional, Rosenbusch, JP, additional, Zulauf, M, additional, and Timmins, PA, additional

Published

1995

4. Collagen-mineral axial relationship in calcified turkey leg tendon by X-ray and neutron diffraction

Author

White, Sw, Hulmes, Dj, Miller, A., Timmins, Pa, and Deleage, Gilbert

Subjects

biological sciences, [SDV.BBM] Life Sciences [q-bio]/Biochemistry, Molecular Biology

Abstract

The axial relationship between the collagen and mineral componetns in calcified turkey leg tendon was investigated using low-angle X-ray and neutron diffraction. The results indicate that the mineral is arranged with the same axial periodicity as the collagen and occupies the gap region of the collagen structure.The axial relationship between the collagen and mineral componetns in calcified turkey leg tendon was investigated using low-angle X-ray and neutron diffraction. The results indicate that the mineral is arranged with the same axial periodicity as the collagen and occupies the gap region of the collagen structure.

Published

1977

5. INTERPRETATION OF THE LOW-ANGLE MERIDIONAL NEUTRON-DIFFRACTION PATTERNS FROM COLLAGEN-FIBERS IN TERMS OF THE AMINO-ACID-SEQUENCE

Author

Hulmes, Djs, Miller, A., White, Sw, Timmins, Pa, Berthetcolominasc, Xxxx, and Deleage, Gilbert

Subjects

[SDV.BBM] Life Sciences [q-bio]/Biochemistry, Molecular Biology

Abstract

xxx

Published

1980

6. A class of mild surfactants that keep integral membrane proteins water-soluble for functional studies and crystallization.

Author

Hovers J, Potschies M, Polidori A, Pucci B, Raynal S, Bonneté F, Serrano-Vega MJ, Tate CG, Picot D, Pierre Y, Popot JL, Nehmé R, Bidet M, Mus-Veteau I, Busskamp H, Jung KH, Marx A, Timmins PA, and Welte W

Subjects

Chlamydomonas reinhardtii chemistry, Cytochrome b6f Complex chemistry, Glucosides chemistry, Humans, Patched Receptors, Receptors, Cell Surface chemistry, Receptors, G-Protein-Coupled chemistry, Solubility, Crystallization methods, Membrane Proteins chemistry, Surface-Active Agents chemistry, Water chemistry

Abstract

Mixed protein-surfactant micelles are used for in vitro studies and 3D crystallization when solutions of pure, monodisperse integral membrane proteins are required. However, many membrane proteins undergo inactivation when transferred from the biomembrane into micelles of conventional surfactants with alkyl chains as hydrophobic moieties. Here we describe the development of surfactants with rigid, saturated or aromatic hydrocarbon groups as hydrophobic parts. Their stabilizing properties are demonstrated with three different integral membrane proteins. The temperature at which 50% of the binding sites for specific ligands are lost is used as a measure of stability and dodecyl-β-D-maltoside ('C12-b-M') as a reference for conventional surfactants. One surfactant increased the stability of two different G protein-coupled receptors and the human Patched protein receptor by approximately 10°C compared to C12-b-M. Another surfactant yielded the highest stabilization of the human Patched protein receptor compared to C12-b-M (13°C) but was inferior for the G protein-coupled receptors. In addition, one of the surfactants was successfully used to stabilize and crystallize the cytochrome b(6 )f complex from Chlamydomonas reinhardtii. The structure was solved to the same resolution as previously reported in C12-b-M.

Published

2011

7. Interaction of cationic lipoplexes with floating bilayers at the solid-liquid interface.

Author

Talbot JP, Barlow DJ, Lawrence MJ, Timmins PA, and Fragneto G

Subjects

Adsorption, Animals, Cattle, DNA metabolism, Lipid Bilayers metabolism, Neutron Diffraction, Phosphatidylcholines chemistry, Polyethylene Glycols chemistry, Silicon Dioxide chemistry, Surface Properties, Lipid Bilayers chemistry

Abstract

Neutron reflection has been used to study the interaction of cationic lipoplexes with different model membrane systems. The model membranes used are prepared as "floating" phospholipid bilayers deposited at a silicon/water interface and separated from the solid substrate either by an adsorbed phospholipid bilayer, polymer cushions composed of polyethylene glycol lipids, or a lipid monolayer adsorbed onto a chemically grafted hydrocarbon layer. The cationic lipoplexes studied are those formed by the complexation of calf thymus DNA with dimethyl-dioctadecylammonium bromide (DDAB), with either cholesterol or dioleoyl-L-alpha-phosphatidylethanolamine (DOPE) incorporated as "helper" lipid. The cationic lipoplexes are found to destroy three of the four types of (negatively charged) floating bilayers, with the rate of destruction dependent on the nature of the layer separating the floating bilayer from the silicon substrate. The only bilayers to remain intact after exposure to the lipoplexes were those fabricated above the chemically grafted (octadecyl) hydrocarbon layer. This supports the hypothesis that the high negative charge density of the SiO2 layer on the silicon surface may influence, by way of electrostatic interaction with the cationic lipid, the interaction of the lipoplexes with the model bilayer. It is concluded that the floating bilayer supported on a chemically grafted hydrocarbon layer lends itself perfectly to the study of lipoplex-membrane interactions and, with sufficient exposure time, would allow a detailed characterization of the structures formed at the membrane interface during the interaction.

Published

2009

8. Selective deuteration of tryptophan and methionine residues in maltose binding protein: a model system for neutron scattering.

Author

Laux V, Callow P, Svergun DI, Timmins PA, Forsyth VT, and Haertlein M

Subjects

Maltose-Binding Proteins, Protein Binding, Staining and Labeling methods, Carrier Proteins chemistry, Deuterium chemistry, Methionine chemistry, Neutron Diffraction methods, Scattering, Small Angle, Tryptophan chemistry

Abstract

We describe methods that have been developed within the ILL-EMBL Deuteration Laboratory for the production of maltose binding protein (MBP) that has been selectively labelled either with deuterated tryptophan or deuterated methionine (single labelling), or both (double labelling). MBP is used as an important model system for biophysical studies, and selective labelling can be helpful in the analysis of small-angle neutron scattering (SANS) data, neutron reflection (NR) data, and high-resolution neutron diffraction data. The selective labelling was carried out in E. coli high-cell density cultures using auxotrophic mutants in minimal medium containing the required deuterated precursors. Five types of sample were prepared and studied: (1) unmodified hydrogenated MBP (H-MBP), (2) perdeuterated MBP (D-MBP), (3) singly labelled MBP with the tryptophan residues deuterated (D-trp MBP), (4) singly labelled MBP with methionine residues deuterated (D-met MBP) and (5) doubly labelled MBP with both tryptophan and methionine residues deuterated (D-trp/met MBP). Labelled samples were characterised by size exclusion chromatography, gel electrophoresis, light scattering and mass spectroscopy. Preliminary small-angle neutron scattering (SANS) experiments have also been carried out and show measurable differences between the SANS data recorded for the various labelled analogues. More detailed SANS experiments using these labelled MBP analogues are planned; the degree to which such data could enhance structure determination by SANS is discussed.

Published

2008

9. Solution structure of the chicken skeletal muscle troponin complex via small-angle neutron and X-ray scattering.

Author

King WA, Stone DB, Timmins PA, Narayanan T, von Brasch AA, Mendelson RA, and Curmi PM

Subjects

Animals, Calcium metabolism, Calcium pharmacology, Models, Molecular, Multiprotein Complexes chemistry, Multiprotein Complexes metabolism, Myocardium chemistry, Protein Binding, Protein Structure, Quaternary drug effects, Protein Subunits chemistry, Protein Subunits metabolism, Solutions chemistry, X-Ray Diffraction, Chickens, Muscle, Skeletal chemistry, Neutron Diffraction, Troponin chemistry, Troponin metabolism

Abstract

Troponin is a Ca2+-sensitive switch that regulates the contraction of vertebrate striated muscle by participating in a series of conformational events within the actin-based thin filament. Troponin is a heterotrimeric complex consisting of a Ca2+-binding subunit (TnC), an inhibitory subunit (TnI), and a tropomyosin-binding subunit (TnT). Ternary troponin complexes have been produced by assembling recombinant chicken skeletal muscle TnC, TnI and the C-terminal portion of TnT known as TnT2. A full set of small-angle neutron scattering data has been collected from TnC-TnI-TnT2 ternary complexes, in which all possible combinations of the subunits have been deuterated, in both the +Ca2+ and -Ca2+ states. Small-angle X-ray scattering data were also collected from the same troponin TnC-TnI-TnT2 complex. Guinier analysis shows that the complex is monomeric in solution and that there is a large change in the radius of gyration of TnI when it goes from the +Ca2+ to the -Ca2+ state. Starting with a model based on the human cardiac troponin crystal structure, a rigid-body Monte Carlo optimization procedure was used to yield models of chicken skeletal muscle troponin, in solution, in the presence and in the absence of regulatory calcium. The optimization was carried out simultaneously against all of the scattering data sets. The optimized models show significant differences when compared to the cardiac troponin crystal structure in the +Ca2+ state and provide a structural model for the switch between +Ca2+ and -Ca2+ states. A key feature is that TnC adopts a dumbbell conformation in both the +Ca2+ and -Ca2+ states. More importantly, the data for the -Ca2+ state suggest a long extension of the troponin IT arm, consisting mainly of TnI. Thus, the troponin complex undergoes a large structural change triggered by Ca2+ binding.

Published

2005

10. Molecular and mesoscale structures in hydrophobically driven aqueous solutions.

Author

Finney JL, Bowron DT, Daniel RM, Timmins PA, and Roberts MA

Subjects

Models, Molecular, Molecular Structure, Proteins chemistry, Solutions chemistry, Thermodynamics, Alcohols chemistry, Hydrophobic and Hydrophilic Interactions, Water chemistry

Abstract

Since Kauzmann's seminal 1959 paper, the hydrophobic interaction has dominated thinking on the forces that control protein folding and stability. Despite its wide importance in chemistry and biology, our understanding of this interaction at the molecular level remains poor, with little experimental evidence to support the idea of water ordering close to a non-polar group that is at the centre of the standard model for the source of the entropic driving force. Developments over recent years in neutron techniques now enable us to see directly how a non-polar group actually affects the molecular structure of the water in its immediate neighbourhood. On the basis of such work on aqueous solutions of small alcohols, the generally accepted standard model is found to be wanting, and alternative sources of the entropic driving force are suggested. Moreover, the fact that we can now follow changes in hydrogen bonding as the alcohol concentration is varied gives us the possibility of explaining the concentration dependence of the enthalpy of mixing. Complementary studies of solute association on the mesoscopic scale show a rich concentration and temperature behaviour, which reflects a complex balance of polar and non-polar interactions. Unravelling the detailed nature of this balance in simple aqueous amphiphiles may lead to a better understanding of the forces that control biomolecular structural stability and interactions.

Published

2003

11. Neutron and X-ray scattering by ox corneal stroma differentially loaded with bound anions.

Author

Regini JW, Timmins PA, Elliott GF, and Hodson SA

Subjects

Animals, Anions, Cattle, Deuterium Oxide chemistry, Male, Neutron Diffraction, Osmolar Concentration, X-Ray Diffraction, Chlorides chemistry, Collagen chemistry, Corneal Stroma chemistry

Abstract

Ox corneas at near physiological hydration were subjected to two variables: the amount of chloride ions bound to them and exposure of various mixtures of H(2)O/D(2)O as solvent. The preparations were then exposed to a neutron beam and the contrast match points, at which the collagen fibrils of the corneal stroma most nearly matched the scattering density of the various H(2)O/D(2)O mixtures, were measured. In both cases of high and low bound chloride, the contrast match points of the collagen fibril were equal, indicating that there were no significant changes in the water of electrostriction at the fibril surface when chloride ions bind to the stroma. The data suggest that the ligands which bind anions to corneal stroma are not located at the collagen fibril surface. When the chloride binding ligands were extracted from the corneal stroma there were significant changes in the structure of the fibrils. We suggest that the chloride binding ligands may be located within the collagen fibril.

Published

2003

12. Detergent organisation in crystals of monomeric outer membrane phospholipase A.

Author

Snijder HJ, Timmins PA, Kalk KH, and Dijkstra BW

Subjects

Crystallography, X-Ray, Deuterium Oxide, Dimerization, Fourier Analysis, Hydrolysis, Micelles, Models, Statistical, Neutrons, Phospholipases A1, Protein Conformation, Scattering, Radiation, Water, Xenon, Bacterial Outer Membrane Proteins chemistry, Bacterial Proteins chemistry, Detergents pharmacology, Phospholipases A chemistry

Abstract

The structure of the detergent in crystals of outer membrane phospholipase A (OMPLA) has been determined using neutron diffraction contrast variation. Large crystals were soaked in stabilising solutions, each containing a different H(2)O/D(2)O contrast. From the neutron diffraction at five contrasts, the 12 A resolution structure of the detergent micelle around the protein molecule was determined. The hydrophobic beta-barrel surfaces of the protein molecules are covered by rings of detergent. These detergent belts are fused to neighbouring detergent rings forming a continuous three-dimensional network throughout the crystal. The thickness of the detergent layer around the protein varies from 7-20 A. The enzyme's active site is positioned just outside the hydrophobic detergent zone and is thus in a proper location to catalyse the hydrolysis of phospholipids in a natural membrane. Although the dimerisation face of OMPLA is covered with detergent, the detergent density is weak near the exposed polar patch, suggesting that burying this patch in the enzyme's dimer interface may be energetically favourable. Furthermore, these results indicate a crucial role for detergent coalescence during crystal formation and contribute to the understanding of membrane protein crystallisation.

Published

2003

13. Hierarchical assembly of the Alu domain of the mammalian signal recognition particle.

Author

Weichenrieder O, Stehlin C, Kapp U, Birse DE, Timmins PA, Strub K, and Cusack S

Subjects

Amino Acid Substitution, Animals, Base Sequence, Mammals, Models, Molecular, Molecular Sequence Data, Mutagenesis, RNA metabolism, RNA-Binding Proteins metabolism, Ribonucleoproteins metabolism, Signal Recognition Particle metabolism, Alu Elements, Nucleic Acid Conformation, RNA chemistry, RNA-Binding Proteins chemistry, Signal Recognition Particle chemistry

Abstract

The mammalian signal recognition particle (SRP) catalytically promotes cotranslational translocation of signal sequence containing proteins across the endoplasmic reticulum membrane. While the S-domain of SRP binds the N-terminal signal sequence on the nascent polypeptide, the Alu domain of SRP temporarily interferes with the ribosomal elongation cycle until the translocation pore in the membrane is correctly engaged. Here we present biochemical and biophysical evidence for a hierarchical assembly pathway of the SRP Alu domain. The proteins SRP9 and SRP14 first heterodimerize and then initially bind to the Alu RNA 5' domain. This creates the binding site for the Alu RNA 3' domain. Alu RNA then undergoes a large conformational change with the flexibly linked 3' domain folding back by 180 degrees onto the 5' domain complex to form the final compact Alu ribonucleoprotein particle (Alu RNP). We discuss the possible mechanistic consequences of the likely reversibility of this final step with reference to translational regulation by the SRP Alu domain and with reference to the structurally similar Alu RNP retroposition intermediates derived from Alu elements in genomic DNA.

Published

2001

14. Effects of ligand binding on the association properties and conformation in solution of retinoic acid receptors RXR and RAR.

Author

Egea PF, Rochel N, Birck C, Vachette P, Timmins PA, and Moras D

Subjects

Apoproteins metabolism, Binding Sites, Computer Simulation, Crystallography methods, Dimerization, Humans, Ligands, Models, Molecular, Mutation, Neutrons, Protein Binding, Protein Conformation, Protein Structure, Quaternary, Protein Structure, Tertiary, Receptors, Retinoic Acid chemistry, Receptors, Retinoic Acid genetics, Retinoid X Receptors, Scattering, Radiation, Solutions, Stereoisomerism, Transcription Factors chemistry, Transcription Factors genetics, Transcriptional Activation, Ultracentrifugation, X-Rays, Receptors, Retinoic Acid metabolism, Transcription Factors metabolism, Tretinoin metabolism

Abstract

In higher eukaryotes, vitamin A derived metabolites such as 9-cis and all-trans retinoic acid (RA), are involved in the regulation of several essential physiological processes. Their pleiotropic physiological effects are mediated through direct binding to cognate nuclear receptors RXRs and RARs that act as regulated transcription factors belonging to the superfamily of nuclear hormone receptors. Hormone binding to the structurally conserved ligand-binding domain (LBD) of these receptors triggers a conformational change that principally affects the conserved C-terminal transactivation helix H12 involved in transcriptional activation. We report an extensive biophysical solution study of RAR alpha, RXR alpha LBDs and their corresponding RXR alpha/RAR alpha LBD heterodimers combining analytical ultracentrifugation (AUC), small-angle X-ray and neutron scattering (SAXS and SANS) and ab initio three-dimensional shape reconstruction at low resolution. We show that the crystal structures of RXRs and RARs LBDs correlate well with the average conformations observed in solution. Furthermore we demonstrate the effects of 9-cisRA and all-transRA binding on the association properties and conformations of RXR alpha and RAR alpha LBDs in solution. The present study shows that in solution RAR alpha LBD behaves as a monomer in both unliganded and liganded forms. It confirms the existence in solution of a ligand-induced conformational change towards a more compact form of the LBD. It also confirms the stability of the predicted RXR alpha/RAR alpha LBD heterodimers in solution. SAS measurements performed on three different types of RXR alpha/RAR alpha LBD heterodimers (apo/apo, apo/holo and holo/holo) with respect to their ligand-binding site occupancy show the existence of three conformational states depending on the progressive binding of RA stereoisomers on RAR alpha and RXR alpha LBD subunits in the heterodimeric context. These results suggest that the subunits are structurally independent within the heterodimers. Our study also underlines the particular behaviour of RXR alpha LBD. In solution unliganded RXR alpha LBD is observed as two species that are unambiguously identified as homotetramers and homodimers. Molecular modelling combined with SAS data analysis allows us to propose a structural model for this autorepressed apo-tetramer. In contrast to the monomeric state observed in the crystal structure, our data show that in solution active holo-RXR alpha LBD bound to 9-cisRA is a homodimer regardless of the protein concentration. This study demonstrates the crucial role of ligands in the regulation of homodimeric versus heterodimeric association state of RXR in the NR signalling pathways., (Copyright 2001 Academic Press.)

Published

2001

15. Small angle neutron scattering and gel filtration analyses of neutrophil NADPH oxidase cytosolic factors highlight the role of the C-terminal end of p47phox in the association with p40phox.

Author

Grizot S, Grandvaux N, Fieschi F, Fauré J, Massenet C, Andrieu JP, Fuchs A, Vignais PV, Timmins PA, Dagher MC, and Pebay-Peyroula E

Subjects

Chromatography, Gel, Cytosol enzymology, Dimerization, HL-60 Cells, Humans, Molecular Weight, Neutrons, Peptide Fragments genetics, Peptide Fragments isolation & purification, Peptide Fragments metabolism, Phosphoproteins genetics, Phosphoproteins isolation & purification, Scattering, Radiation, Solutions, NADPH Oxidases metabolism, Neutrophils enzymology, Peptide Fragments physiology, Phosphoproteins metabolism, Phosphoproteins physiology

Abstract

The NADPH oxidase of phagocytic cells is regulated by the cytosolic factors p47(phox), p67(phox), and p40(phox) as well as by the Rac1-Rho-GDI heterodimer. The regulation is a consequence of protein-protein interactions involving a variety of protein domains that are well characterized in signal transduction. We have studied the behavior of the NADPH oxidase cytosolic factors in solution using small angle neutron scattering and gel filtration. p47(phox), two truncated forms of p47(phox), namely, p47(phox) without its C-terminal end (residues 1-358) and p47(phox) without its N-terminal end (residues 147-390), and p40(phox) were found to be monomeric in solution. The dimeric form of p67(phox) previously observed by gel filtration experiments was confirmed. Our small angle neutron scattering experiments show that p40(phox) binds to the full-length p47(phox) in solution in the absence of phosphorylation. We demonstrated that the C-terminal end of p47(phox) is essential in this interaction. From the comparison of the presence or absence of interaction with various truncated forms of the proteins, we confirmed that the SH3 domain of p40(phox) interacts with the C-terminal proline rich region of p47(phox). The radii of gyration observed for p47(phox) and the truncated forms of p47(phox) (without the C-terminal end or without the N-terminal end) show that all these molecules are elongated and that the N-terminal end of p47(phox) is globular. These results suggest that the role of amphiphiles such as SDS or arachidonic acid or of p47(phox) phosphorylation in the elicitation of NADPH oxidase activation could be to disrupt the p40(phox)-p47(phox) complex rather than to break an intramolecular interaction in p47(phox).

Published

2001

16. Studies on the structure and mechanism of a bacterial protein toxin by analytical ultracentrifugation and small-angle neutron scattering.

Author

Gilbert RJ, Heenan RK, Timmins PA, Gingles NA, Mitchell TJ, Rowe AJ, Rossjohn J, Parker MW, Andrew PW, and Byron O

Subjects

Amino Acid Sequence, Bacterial Proteins, Cytotoxins genetics, Dimerization, Lipid Bilayers chemistry, Liposomes chemistry, Models, Molecular, Molecular Sequence Data, Mutation genetics, Neutrons, Protein Binding, Protein Structure, Quaternary, Scattering, Radiation, Solutions, Streptococcus pneumoniae chemistry, Streptococcus pneumoniae genetics, Streptolysins genetics, Structure-Activity Relationship, Ultracentrifugation, Water metabolism, Cytotoxins chemistry, Cytotoxins metabolism, Lipid Bilayers metabolism, Liposomes metabolism, Streptolysins chemistry, Streptolysins metabolism

Abstract

Pneumolysin, an important virulence factor of the human pathogen Streptococcus pneumoniae, is a pore-forming toxin which also possesses the ability to activate the complement system directly. Pneumolysin binds to cholesterol in cell membrane surfaces as a prelude to pore formation, which involves the oligomerization of the protein. Two important aspects of the pore-forming activity of pneumolysin are therefore the effect of the toxin on bilayer membrane structure and the nature of the self-association into oligomers undergone by it. We have used analytical ultracentrifugation (AUC) to investigate oligomerization and small-angle neutron scattering (SANS) to investigate the changes in membrane structure accompanying pore formation. Pneumolysin self-associates in solution to form oligomeric structures apparently similar to those which appear on the membrane coincident with pore formation. It has previously been demonstrated by us using site-specific chemical derivatization of the protein that the self-interaction preceding oligomerization involves its C-terminal domain. The AUC experiments described here involved pneumolysin toxoids harbouring mutations in different domains, and support our previous conclusions that self-interaction via the C-terminal domain leads to oligomerization and that this may be related to the mechanism by which pneumolysin activates the complement system.SANS data at a variety of neutron contrasts were obtained from liposomes used as model cell membranes in the absence of pneumolysin, and following the addition of toxin at a number of concentrations. These experiments were designed to allow visualization of the effect that pneumolysin has on bilayer membrane structure resulting from oligomerization into a pore-forming complex. The structure of the liposomal membrane alone and following addition of pneumolysin was calculated by the fitting of scattering equations directly to the scattering curves. The fitting equations describe scattering from simple three-dimensional scattering volume models for the structures present in the sample, whose dimensions were varied iteratively within the fitting program. The overall trend was a thinning of the liposome surface on toxin attack, which was countered by the formation of localized structures thicker than the liposome bilayer itself, in a manner dependent on pneumolysin concentration. At the neutron contrast match point of the liposomes, pneumolysin oligomers were observed. Inactive toxin appeared to bind to the liposome but not to cause membrane alteration; subsequent activation of pneumolysin in situ brought about changes in liposome structure similar to those seen in the presence of active toxin. We propose that the changes in membrane structure on toxin attack which we have observed are related to the mechanism by which pneumolysin forms pores and provide an important perspective on protein/membrane interactions in general. We discuss these results in the light of published data concerning the interaction of gramicidin with bilayers and the hydrophobic mismatch effect., (Copyright 1999 Academic Press.)

Published

1999

17. Depletion interaction of casein micelles and an exocellular polysaccharide.

Author

Tuinier R, ten Grotenhuis E, Holt C, Timmins PA, and de Kruif CG

Subjects

Cell Adhesion, Electron Spin Resonance Spectroscopy, Lactococcus lactis metabolism, Light, Models, Statistical, Scattering, Radiation, Caseins chemistry, Micelles, Polysaccharides chemistry

Abstract

Casein micelles become mutually attractive when an exocellular polysaccharide produced by Lactococcus lactis subsp. cremoris NIZO B40 (hereafter called EPS) is added to skim milk. The attraction can be explained as a depletion interaction between the casein micelles induced by the nonadsorbing EPS. We used three scattering techniques (small-angle neutron scattering, turbidity measurements, and dynamic light scattering) to measure the attraction. In order to connect the theory of depletion interaction with experiment, we calculated structure factors of hard spheres interacting by a depletion pair potential. Theoretical predictions and all the experiments showed that casein micelles became more attractive upon increasing the EPS concentration.

Published

1999

18. The effect of regulatory Ca2+ on the in situ structures of troponin C and troponin I: a neutron scattering study.

Author

Stone DB, Timmins PA, Schneider DK, Krylova I, Ramos CH, Reinach FC, and Mendelson RA

Subjects

Animals, Ca(2+) Mg(2+)-ATPase chemistry, Calcium-Binding Proteins chemistry, Models, Molecular, Muscle Proteins chemistry, Muscle, Skeletal physiology, Neutrons, Protein Binding, Rabbits, Recombinant Proteins chemistry, Calcium pharmacology, Troponin C chemistry, Troponin I chemistry

Abstract

The effects of regulatory amounts of Ca2+ on the in situ structures of troponin C (TnC) and troponin I (TnI) in whole troponin have been investigated by neutron scattering. In separate difference experiments, 97% deuterated TnC and TnI within whole troponin were studied +/-Ca2+ in 41.6% 2H2O buffers in which protonated subunits were rendered "invisible". We found that the radius of gyration (Rg) of TnI decreased by approximately 10% upon addition of regulatory Ca2+ indicating that it was significantly more compact in the presence of Ca2+. The apparent cross-sectional radius of gyration (Rc) of TnI increased by about 9% when regulatory Ca2+ was bound to TnC. Modeling studies showed that the high-Q scattering patterns of TnI could be fit by a TnI which consisted of two subdomains: one, a highly oblate ellipsoid of revolution containing about 65% of the mass and the other, a highly prolate ellipsoid of revolution consisting of about 35% of the mass. No other fits could be found with this class of models. Best fits were achieved when the axes of revolution of these ellipsoids were steeply inclined with respect to each other. Ca2+ addition decreased the center of mass separation by about 1.5 nm. The Rg of TnI, its high-Q scattering pattern, and the resultant structure were different from previous results on neutron scattering by TnI in the (+Ca2+) TnC.TnI complex. The Rg of TnC indicated that it was elongate in situ. The Rg of TnC was not sensitive to the Ca2+ occupancy of its regulatory sites. However, Rc increased upon Ca2+ addition in concert with expectations from NMR and crystallography of isolated TnC. The present observations indicate that TnI acts like a molecular switch which is controlled by smaller Ca2+-induced changes in TnC., (Copyright 1998 Academic Press.)

Published

1998

19. Detergent binding in trigonal crystals of OmpF porin from Escherichia coli.

Author

Penel S, Pebay-Peyroula E, Rosenbusch J, Rummel G, Schirmer T, and Timmins PA

Subjects

Crystallization, Crystallography methods, Crystallography, X-Ray, Detergents chemistry, Detergents metabolism, Models, Molecular, Neutrons, Escherichia coli chemistry, Porins chemistry, Porins metabolism, Sulfoxides chemistry, Sulfoxides metabolism

Abstract

The structure of the detergent, ocytyl hydroxyethylsufoxide (C8(HE)SO), bound to the OmpF porin from E coli (in the trigonal crystal form) has been determined by neutron crystallography. Due to a dynamic exchange of detergent molecules with their environment they are not ordered on an atomic scale. The structure reported here is therefore at a resolution of approximately 16 A. The X-ray crystallographically determined structure of the protein provides a starting point for the neutron analysis in which the detergent is visualized primarily thanks to its high contrast against D2O. The structure shows the detergent to be located mainly in two areas. It forms toroidal annuli around each OmpF trimer, these annuli fusing to form a detergent belt surrounding a solvent filled column traversing the crystal. Those areas of the protein to which the detergent binds are formed almost exclusively of hydrophobic residues and form a band about 30 A high around the trimer. Its upper and lower bounds are defined by two bands of aromatic residues, tyrosines pointing away from the detergent belt and interacting with the polar headgroups while phenylalanines point inwards. This strongly suggests that the same areas define, in vivo, the location at which protein interacts with lipid. The hydrophobic moiety of detergent is also found mediating the hydrophobic protein-protein interactions at the interface between two trimers on the crystallographic two-fold axis.

Published

1998

20. A core-shell model of calcium phosphate nanoclusters stabilized by beta-casein phosphopeptides, derived from sedimentation equilibrium and small-angle X-ray and neutron-scattering measurements.

Author

Holt C, Timmins PA, Errington N, and Leaver J

Subjects

Micelles, Molecular Conformation, Molecular Weight, Neutrons, Peptide Fragments pharmacology, Phosphopeptides isolation & purification, Scattering, Radiation, Ultracentrifugation, X-Rays, Calcium Phosphates chemistry, Caseins chemistry, Phosphopeptides pharmacology

Abstract

Calcium phosphate nanoclusters were prepared under standardised conditions using 10 mg ml(-1) of the 25-amino-acid N-terminal tryptic phosphopeptide of bovine beta-casein as a stabilising agent. The Mr determined by sedimentation equilibrium was 197,600+/-13,700 and the apparent radius of gyration determined by X-ray scattering was 2.80+/-0.05 nm. A small-angle neutron scattering contrast variation study in 1H2O/2H2O mixtures was performed and gave radii of gyration at the calculated match points for the calcium phosphate (88.2% 2H2O) and phosphopeptide (41.3% 2H2O) of 3.39+/-0.08 nm and 1.85+/-0.05 nm, respectively. Measurements at larger scattering wave vector showed a subsidiary maximum at about Q = 1.6 nm(-1). The results are consistent with a model of the nanoclusters comprising a spherical core of 355+/-20 CaHPO4 x 2 H2O units, density 2.31 g ml(-1) and radius 2.30+/-0.05 nm surrounded by 49+/-4 peptide chains with a partial specific volume of 0.7 cm3 g(-1), forming a tightly packed shell with an outer radius of 4.04+/-0.15 nm. This model suggests that the phosphopeptide is able to arrest the process of growth of the precipitating phase of calcium phosphate at its earliest stages. A similar role for whole casein could be vital to the normal functioning of the mammary gland during milk secretion.

Published

1998

21. Protein-detergent interactions in single crystals of membrane proteins studied by neutron crystallography.

Author

Timmins PA and Pebay-Peyroula E

Subjects

Crystallography methods, Escherichia coli, Models, Structural, Neutrons, Photosynthetic Reaction Center Complex Proteins chemistry, Porins chemistry, Rhodobacter, Rhodopseudomonas, Detergents, Membrane Proteins chemistry, Protein Conformation

Abstract

The detergent micelles surrounding membrane protein molecules in single crystals can be investigated using neutron crystallography combined with H2O/D2O contrast variation. If the protein structure is known then the contrast variation method allows phases to be determined at a contrast where the detergent dominates the scattering. The application of various constraints allows the resulting scattering length density map to be realistically modeled. The method has been applied to two different forms of the membrane protein porin. In one case both hydrogenated and partially deuterated protein were used, allowing the head group and tail to be distinguished.

Published

1996

22. The three-dimensional distribution of RNA and protein in the interior of tomato bushy stunt virus: a neutron low-resolution single-crystal diffraction study.

Author

Timmins PA, Wild D, and Witz J

Subjects

Crystallography, X-Ray, Neutrons, Protein Conformation, RNA, Viral chemistry, Tombusvirus genetics, Viral Proteins chemistry, RNA, Viral metabolism, Tombusvirus metabolism, Viral Proteins metabolism

Abstract

Background: The published high-resolution model of the isometric T = 3 plant virus tomato bushy stunt virus (TBSV) shows the packing in three different environments (A, B, C) of the 180 coat protein subunits of the capsid. It does not, however, account for the localization of either the viral RNA or approximately 25% of the amino acids of the protein subunits, although at least the RNA is rigidly linked to the viral capsid. Solution studies have shown that most of the missing protein is located in an inner shell, and that most of the RNA is sandwiched between the two protein shells., Results: We have determined the organization of TBSV at 16 A resolution, using neutron single-crystal diffraction. Connections between the two protein shells are confined to the 20 three-fold axes of the virion, where three C-type subunits meet. Much more RNA density is located under the 30 C-C dimers than under the 60 A-B dimers, where we could even identify lagoons of solvent., Conclusions: Our results emphasize the importance of the amino termini of the 60 C-type protein subunits not only in the RNA-protein interactions but also in the organization of the coat protein, and, probably, in the assembly of the virion. The lack of equivalence between subunits of classes A or B and subunits of class C is even more pronounced in the interior of the virion than in the outer shell, which possesses icosahedral symmetry.

Published

1994

23. Membrane-bound form of the pore-forming domain of colicin A. A neutron scattering study.

Author

Jeanteur D, Pattus F, and Timmins PA

Subjects

Membrane Proteins chemistry, Membrane Proteins ultrastructure, Neutrons, Peptide Fragments chemistry, Phosphatidylglycerols chemistry, Protein Structure, Secondary, Scattering, Radiation, Colicins ultrastructure, Ion Channels ultrastructure

Abstract

The ion-channel forming C-terminal fragment of colicin A binds to negatively charged lipid vesicles and provides an example of the insertion of a soluble protein into a lipid bilayer. The soluble structure is known and consists of a ten-helix bundle containing a hydrophobic helical hairpin. This fragment forms a well-defined complex with dimyristoylphosphatidyl-glycerol which is thus amenable to neutron scattering studies. Neutron scattering experiments in the Guinier range (low angles) provided the mass and the stoichiometry of the complex (290,000 (+/- 10,000) M(r), 8.2 (+/- 0.5)), in fair agreement with previous determinations. By varying the neutron scattering length density of the solvent with 2H2O/H2O mixtures and therefore the contrast of the different components, the radial distribution of the protein and of the lipids was determined. Finally, an attempt was made to fit various models to the wider angle scattering data. This study suggests that the pore-forming fragment of colicin A lies mostly at the surface of the membrane, with the lipids arranged in a bilayer organization.

Published

1994

24. Organization of turnip yellow mosaic virus investigated by neutron small angle scattering at 80 K: an intermediate state preceding decapsidation of the virion?

Author

Witz J, Timmins PA, and Adrian M

Subjects

Capsid ultrastructure, Freezing, Neutrons, RNA, Viral ultrastructure, Scattering, Radiation, Tymovirus ultrastructure, Virion ultrastructure

Abstract

The organization of turnip yellow mosaic virus has been investigated by neutron small angle scattering at 300 K and 80 K in buffers containing various amounts of D2O. We confirm that in native virions, no substantial part of the RNA is located at a radius larger than ca. 100-110 A, i.e., that there is very little interpretation of the RNA into the capsid. At 80 K, scattering curves do not depend much upon contrast, from 40% D2O to 100% D2O buffers, but are strongly affected by interparticle interference. We could, however, show that it is not the case for the subsidiary intensity maximum at q approximately 0.06 A-1. From the position of this maximum, we conclude that upon freezing, the radius of the capsid expands by c.a. 3.5% and the RNA penetrates deeply into the protein shell. Biological implications of this conformational change immediately preceding decapsidation are discussed.

Published

1993

25. Activation of recA protein. The open helix model for LexA cleavage.

Author

DiCapua E, Cuillel M, Hewat E, Schnarr M, Timmins PA, and Ruigrok RW

Subjects

Adenosine Triphosphate analogs & derivatives, Adenosine Triphosphate metabolism, Adenosine Triphosphate pharmacology, DNA, Bacterial chemistry, DNA, Bacterial ultrastructure, Heparin pharmacology, Kinetics, Microscopy, Electron, Models, Structural, Plasmids, Protein Conformation, RNA, Transfer chemistry, Rec A Recombinases chemistry, Rec A Recombinases ultrastructure, Bacterial Proteins metabolism, Coliphages metabolism, DNA, Bacterial metabolism, Escherichia coli metabolism, RNA, Transfer metabolism, Rec A Recombinases metabolism, Serine Endopeptidases

Abstract

RecA protein is induced by the binding of DNA and ATP to become active in the hydrolysis of ATP and the cleavage of repressors. These reactions appear to depend on the structural state of the protein polymerized along the DNA, i.e. a helical coat of six RecA per turn of 95 to 100 A pitch. In support of this model of the active conformation, it was shown that high concentrations of salt also induce this helical polymerized state as well as the enzymatic activities. Here, we describe that, in vitro and with the non-hydrolyzable analogue ATP gamma S, RNA and heparin can also induce both the structural transition and the enzymatic activation of RecA to LexA cleavage in accordance with the model. RNA and heparin do not support the reaction in the presence of ATP, and they do not induce the hydrolysis of ATP either, suggesting that, in contrast to ATP gamma S, the nucleotide is not bound stably enough, and that the combined affinities of polynucleotide and ATP actually modulate the discrimination of RecA for the various possible inducers in vivo.

Published

1992

26. In vitro decapsidation of turnip yellow mosaic virus investigated by cryo-electron microscopy: a model for the decapsidation of a small isometric virus.

Author

Adrian M, Timmins PA, and Witz J

Subjects

Capsid metabolism, Cryoultramicrotomy, Microscopy, Electron, Models, Biological, Mosaic Viruses metabolism, RNA, Viral ultrastructure, Vegetables microbiology, Capsid ultrastructure, Mosaic Viruses ultrastructure

Abstract

The in vitro decapsidation of a small isometric plant virus, turnip yellow mosaic virus (TYMV), was investigated by cryo-electron microscopy. Cryo-electron micrographs of TYMV and empty shells show that rapidly frozen virions still contain their RNA. Images of vitrified virions resemble closely those previously obtained by negative staining. Rapidly frozen virions decapsidate upon thawing although they remain well dispersed on the grid. The escape of the RNA through a hole at the periphery of the capsid could be visualized. The results suggest a model for the in situ decapsidation of small icosahedral viruses.

Published

1992

27. The location of bound lipid in the lipovitellin complex.

Author

Timmins PA, Poliks B, and Banaszak L

Subjects

Binding Sites, Chemical Phenomena, Chemistry, Physical, Crystallography, Deuterium, Egg Proteins, Egg Proteins, Dietary metabolism, Lipids analysis, Macromolecular Substances, Molecular Structure, Neutrons, Protein Conformation, Water, X-Ray Diffraction, Egg Proteins, Dietary chemistry, Lipid Metabolism

Abstract

The location of the bound lipid in the soluble lipoprotein lipovitellin has been determined by neutron crystallographic techniques. With the use of the contrast variation method, whereby the crystals are soaked in different H2O-D2O mixtures, the lipid has been found to occupy a large cavity in the protein whose structure had previously been determined by x-ray crystallography. The lipid appears to be bound in the form of a bilayer with the major protein-lipid interactions being hydrophobic and with the lipid headgroups projecting into the bulk solvent and into a solvent-filled space in the cavity.

Published

1992

28. Structure and RNA content of the prosomes.

Author

Coux O, Nothwang HG, Scherrer K, Bergsma-Schutter W, Arnberg AC, Timmins PA, Langowski J, and Cohen-Addad C

Subjects

Animals, Ducks, Electrophoresis, Polyacrylamide Gel, Erythrocytes chemistry, Erythrocytes ultrastructure, Light, Microscopy, Electron, Neutrons, RNA ultrastructure, Ribonucleases metabolism, Scattering, Radiation, RNA chemistry, Ribonucleoproteins genetics

Abstract

Duck erythroblasts prosomes were analysed by small angle neutron scattering (SANS), dynamic light scattering and (cryo-)electron microscopy. A molecular weight of approximately 720,000 +/- 50,000, a radius of gyration of 64 +/- 2 A and a hydrodynamic radius of approximately 86 A were obtained. Electron micrographs show a hollow cylinder-like particle with a diameter of 120 A, a height of 170 A and a diameter of 40 A for the cavity, built of four discs, the two outer ones being more pronounced than those in the center. Results from SANS indicate less then 5% of RNA in the purified prosomes, but nuclease protection assays confirm its presence.

Published

1992

29. Symmetry, flexibility and permeability in the structure of yeast retrotransposon virus-like particles.

Author

Burns NR, Saibil HR, White NS, Pardon JF, Timmins PA, Richardson SM, Richards BM, Adams SE, Kingsman SM, and Kingsman AJ

Subjects

Genes, Viral, Image Processing, Computer-Assisted, Microscopy, Electron, RNA, Fungal genetics, Retroviridae ultrastructure, Transcription, Genetic, Ultracentrifugation, DNA Transposable Elements, Retroviridae genetics, Saccharomyces cerevisiae genetics

Abstract

The virus-like particles (VLPs) of the yeast retrotransposon Ty are genetically, structurally and functionally analogous to retroviral nucleocapsids or cores. Like retroviral cores Ty-VLPs package and possibly promote the enzyme activities for reverse transcription and integration, as well as encapsulating the RNA that is the intermediate in retrotransposition. Here we show that Ty-VLPs assemble into symmetrical structures across a broad distribution of particle sizes. This spread of sizes violates the principle of quasi-equivalent packing. In addition, RNase accessibility experiments suggest that these particles form an open structure that does not protect the encapsulated RNA. These features distinguish Ty-VLPs from typical spherical viral capsids in both structure and function.

Published

1992

30. The influence of heptane-1,2,3-triol on the size and shape of LDAO micelles. Implications for the crystallisation of membrane proteins.

Author

Timmins PA, Hauk J, Wacker T, and Welte W

Subjects

Neutrons, X-Ray Diffraction, Dimethylamines, Fatty Alcohols metabolism, Membrane Proteins chemistry, Micelles

Abstract

The presence of small amphiphiles has been found to be necessary in the crystallization of several membrane-protein/surfactant complexes. It has been suggested that the role of the small amphiphile may be to reduce the size of the surfactant belt around the protein, making the formation of crystals easier. Thus far it was not known if this would involve changes in micellar size in general or whether the small amphiphile would merely replace LDAO during crystal growth. In the present study we have used small angle neutron scattering to study mixed micelles of lauryldimethyl amine oxide (LDAO; hydrogenated and deuterated) and heptane-1,2,3-triol (HP). Our results show that with increasing overall HP concentrations mixed LDAO/HP micelles of decreasing mass and radius are formed. The composition of these micelles has been determined. HP thus may decrease the size of the surfactant belt around a protein before crystallisation by insertion into a host micelle. As HP is a 'small amphiphile' compared to the surfactants used for solubilization of membrane proteins, the curvature of the host micelle will be increased by its insertion.

Published

1991

31. Human adenovirus serotype 3 fiber protein. Comparison of native and recombinant proteins.

Author

Albiges-Rizo C, Barge A, Ruigrok RW, Timmins PA, and Chroboczek J

Subjects

Blotting, Western, Capsid ultrastructure, Cells, Cultured, Cross-Linking Reagents, Electrophoresis, Polyacrylamide Gel, Microscopy, Electron, Plasmids, Adenoviridae metabolism, Capsid chemistry, Capsid Proteins, Viral Proteins chemistry

Abstract

We were able to isolate viral fiber and penton from Ad3-infected KB cells using for their detection antibodies obtained against recombinant Ad3 fiber. The native material was examined by electron microscopy and the characteristic fiber shape of a shaft terminated by a globular head was observed. The native fiber was compared with two recombinant fibers synthesized in Escherichia coli cells. One, the Ad3 fiber protein expressed in E. coli with a 14-amino acid NH2-terminal fusion peptide, under the control of the T7 promoter has been described previously. The second is a recombinant Ad3 fiber without the fusion peptide (recAd3fib), expressed in the same system. As with the fusion protein recAd3fib was found to be insoluble upon expression. It was solubilized in 6 M urea and the gradual removal of urea during the purification cycle led to a soluble preparation. Biochemical and biophysical studies show that, similarly to fusion fiber, recAd3fib self-assembles as trimers in prokaryotic cells. Electron microscopy shows that, whereas the fusion fiber consists of a population of heterogeneous particles, recAd3fib has the characteristic morphology and size of the Ad3 trimeric native fiber. Small angle neutron scattering gives a molecular weight consistent with a trimeric fiber and a radius of gyration consistent with the dimensions derived from electron microscopy. These results suggest that the fusion peptide at the NH2 terminus prevents correct protein folding. They also indicate that after solubilization with urea and subsequent renaturation a correctly folded eukaryotic oligomeric protein can be produced in E. coli.

Published

1991

32. The solution structure of recA filaments by small angle neutron scattering.

Author

Timmins PA, Ruigrok RW, and DiCapua E

Subjects

Crystallization, DNA metabolism, Macromolecular Substances, Neutrons, Protein Conformation, Rec A Recombinases metabolism, Scattering, Radiation, Solutions, Rec A Recombinases chemistry

Abstract

The technique of small angle neutron scattering has been applied to study the structure in solution of recA self-polymers and various recA-DNA complexes. These results are compared with those recently obtained by other physical techniques.

Published

1991

33. Complexes of RecA protein in solution. A study by small angle neutron scattering.

Author

DiCapua E, Schnarr M, Ruigrok RW, Lindner P, and Timmins PA

Subjects

Adenosine Triphosphate, Chemical Phenomena, Chemistry, Physical, DNA, Microscopy, Electron, Neutrons, Scattering, Radiation, Rec A Recombinases ultrastructure

Abstract

RecA complexes on DNA and self-polymers were analysed by small-angle neutron scattering in solution. By Guinier analysis at small angles and by model analysis of a subsidiary peak at wider angles, we find that the filaments fall into two groups: the DNA complex in the presence of ATP gamma S, an open helix with pitch 95 A, a cross-sectional radius of gyration of 33 A and a mass per length of about six RecA units per turn, which corresponds to the state of active enzyme; and the compact form (bound to single-stranded DNA in the absence of ATP, or binding ATP gamma S in the absence of DNA, or just the protein on its own), a helical structure with pitch 70 A, cross-sectional radius of gyration 40 A and mass per length about five RecA units per turn, which corresponds to the conditions of inactive enzyme. The results are discussed in the perspective of unifying previous conflicting structural results obtained by electron microscopy.

Published

1990

34. Activation of recA protein: the salt-induced structural transition.

Author

DiCapua E, Ruigrok RW, and Timmins PA

Subjects

Acetates pharmacology, Acetic Acid, Adenosine Triphosphatases metabolism, Adenosine Triphosphate analogs & derivatives, Adenosine Triphosphate pharmacology, Bacterial Proteins metabolism, Escherichia coli metabolism, Microscopy, Electron, Models, Structural, Neutrons, Osmolar Concentration, Protein Conformation, Rec A Recombinases metabolism, Repressor Proteins metabolism, Scattering, Radiation, Adenosine Triphosphate metabolism, Rec A Recombinases ultrastructure, Serine Endopeptidases

Abstract

Purified recA protein is induced by high salt concentrations to hydrolyse ATP even in the absence of DNA. By small angle neutron scattering we show that this salt activation results from a structural transition of the protein filament in the presence of ATP gamma S from the inactive, compact form (a helical polymer of pitch 70 A and cross-sectional radius of gyration Rc 40 A) to the open form (a helical filament of pitch 95 A and Rc 35 A, which are the same structural parameters as in the ATPase active complex with DNA and ATP), without detectable change in the degree of association. We conclude that activation of recA is due to the same structural change whether induced by the binding of DNA or by salt. Indeed, the other enzymatic activity of recA, the proteolytic cleavage of the lexA repressor, is found to be inducible by the same salt concentrations as those of the structural transition.

Published

1990

35. Molecular weight determination of an active photosystem I preparation from a thermophilic cyanobacterium, Synechococcus elongatus.

Author

Schafheutle ME, Setliková E, Timmins PA, Johner H, Gutgesell P, Setlik I, and Welte W

Subjects

Amino Acids analysis, Cell Membrane analysis, Electron Probe Microanalysis, Light-Harvesting Protein Complexes, Molecular Weight, Neutrons, Photosynthetic Reaction Center Complex Proteins, Photosystem I Protein Complex, Photosystem II Protein Complex, Phycobilisomes, Chlorophyll analysis, Cyanobacteria analysis, Plant Proteins analysis

Abstract

An active photosystem I (PSI) complex was isolated from the thermophilic cyanobacterium Synechococcus elongatus by a procedure consisting of three steps: First, extraction of photosystem II from the thylakoids by a sulfobetaine detergent yields PSI-enriched membranes. Second, the latter are treated with Triton X-100 to extract PSI particles, which are further purified by preparative isoelectric focusing. Third, anion-exchange chromatography is used to remove contaminating phycobilisome polypeptides. The purified particles show three major bands in sodium dodecyl sulfate gel electrophoresis of apparent molecular mass of 110, 15, and 10 kDa. Charge separation was monitored by the kinetics of flash-induced absorption changes at 820 nm. A chlorophyll/P700 ratio of 60 was found. When the particles are stored at 4 degrees C, charge separation was stable for weeks. The molecular mass of the PSI particles, determined by measurement of zero-angle neutron scattering intensity, was 217,000 Da. The PSI particles thus consist of one heterodimer of the 60-80-kDa polypeptides and presumably one copy of the 15- and 10-kDa polypeptides, respectively.

Published

1990

36. Collagen-mineral axial relationship in calcified turkey leg tendon by X-ray and neutron diffraction.

Author

White SW, Hulmes DJ, Miller A, and Timmins PA

Subjects

Animals, Calcification, Physiologic, Neutrons, Protein Conformation, Scattering, Radiation, Turkeys, X-Ray Diffraction, Calcium, Collagen, Tendons ultrastructure

Abstract

The axial relationship between the collagen and mineral componetns in calcified turkey leg tendon was investigated using low-angle X-ray and neutron diffraction. The results indicate that the mineral is arranged with the same axial periodicity as the collagen and occupies the gap region of the collagen structure.

Published

1977

37. Effects of pH and ionic strength on the structure of collagen fibrils.

Author

Ripamonti A, Roveri N, Braga D, Hulmes DJ, Miller A, and Timmins PA

Subjects

Animals, Hydrogen-Ion Concentration, Osmolar Concentration, Protein Conformation, Rats, X-Ray Diffraction, Collagen

Published

1980

38. Neutron diffraction by surface acoustic waves.

Author

Hamilton WA, Klein AG, Opat GI, and Timmins PA

Published

1987

39. Neutron Crystallography of a Membrane Protein: Localization of Detergent and Protein at 20-å Resolution.

Author

Zulauf M, Timmins PA, and Garavito RM

Published

1986

40. Neutron diffraction studies of the corneal stroma.

Author

Elliott GF, Sayers Z, and Timmins PA

Subjects

Animals, Cattle, Collagen analysis, Hydrogen-Ion Concentration, Neutrons, Spectrum Analysis, X-Ray Diffraction, Cornea ultrastructure

Published

1982

41. Bone water.

Author

Timmins PA and Wall JC

Subjects

Absorption, Age Factors, Animals, Apatites, Body Water physiology, Calcium Phosphates, Capillaries, Collagen, Female, Homeostasis, Humans, Male, Molecular Conformation, Osteomalacia pathology, Sex Factors, Temperature, Body Water analysis, Bone and Bones analysis

Abstract

A short review is given of the water in bone. Various analyses of bone water content are discussed, and its possible location is considered in relation to the behaviour of water in isolated components of bone. Some of the difficulties encountered in examining such microscopic phenomena as water structure in a heterogeneous system such as bone are also discussed.

Published

1977

42. Molecular weight and shape of angiotensin-I converting enzyme. A neutron scattering study.

Author

Baudin B, Timmins PA, Drouet L, Legrand Y, and Baumann FC

Subjects

Amino Acids analysis, Animals, Carbohydrates analysis, Lung enzymology, Molecular Weight, Neutrons, Protein Conformation, Scattering, Radiation, Swine, Peptidyl-Dipeptidase A isolation & purification

Abstract

The molecular weight of angiotensin-I converting enzyme from pig lung has been determined to be 112000 (+/- 6000) by neutron scattering. This is somewhat lower than the value determined by SDS-PAGE and than previous estimates which, however, show a very wide range of values. A quantitative analysis of the amino acid and carbohydrate content was made in order to determine the enzyme concentration. The small angle neutron scattering technique also gives information on the molecular shape, yielding a radius of gyration of 44.5 +/- 1.5 A which, for the observed molecular weight, indicates that the angiotensin converting enzyme molecule is clearly elongated in aqueous solution. Dynamic light scattering experiments confirm this conclusion.

Published

1988

43. Crystal packing and stoichiometry of the fibre protein of adenovirus type 2.

Author

Devaux C, Berthet-Colominas C, Timmins PA, Boulanger P, and Jacrot B

Subjects

Crystallization, Microscopy, Electron, Models, Structural, Protein Conformation, X-Ray Diffraction, Adenoviridae analysis, Capsid, Capsid Proteins

Abstract

Crystals of the fibre protein of adenovirus type 2 have been grown and studied by electron microscopy and X-ray powder diffraction. The molecular packing and density of the crystals suggest that the fibre is dimeric.

Published

1984

44. Structural studies of adenovirus type 2 and an assembly mutant.

Author

Berthet-Colominas C, Boulanger P, Devaux C, Jacrot B, and Timmins PA

Published

1986

45. Packaging of DNA in cauliflower mosaic virus and bacteriophage SD studied with magnetic birefringence.

Author

Torbet J, Timmins PA, and Lvov Y

Abstract

Magnetic birefringence measurements are reported on solutions of two double-stranded DNA containing viruses: icosahedral cauliflower mosaic virus (CaMV) and SD, an isometric bacteriophage with a short tail. Assuming the signal comes predominantly from the DNA, constraints can be put on its packing geometry. The anisotropy of CaMV is consistent with the DNA having a near orthogonally wound spool-like structure. The DNA anisotropy is smaller in SD but is compatible with a spool-like structure if the windings are tilted about the spool axis or if a significant proportion of the DNA is effectively isotropically packed. Intermediate structures are also possible.

Published

1986

46. The structure of rice dwarf virus determined by small-angle neutron scattering measurements.

Author

Inoue H and Timmins PA

Abstract

The structure of rice dwarf virus (RDV) has been investigated by small-angle neutron-scattering measurements using the contrast variation method. The contrast match point gave an RNA content of about 20% by weight. The value of the neutron intensity scattered at zero angle in water divided by the virus concentration yielded a particle weight of 65.2 x 10(6). The data suggest that the viral RNA is located at radii

Published

1985

47. Low resolution structures of biological complexes studied by neutron scattering.

Author

Timmins PA and Zaccai G

Subjects

Membranes analysis, Nucleoproteins analysis, Ribosomes analysis, Scattering, Radiation, Viruses analysis, Macromolecular Substances analysis, Neutrons

Published

1988

48. Crystals of glutamine synthetase from Escherichia coli.

Author

Bywater RP, Carlisle CH, Jackson RB, Mackay AL, and Timmins PA

Subjects

Ammonium Sulfate, Crystallization, Mathematics, Microscopy, Electron, Models, Structural, X-Ray Diffraction, Escherichia coli enzymology, Glutamate-Ammonia Ligase

Published

1975

49. Structure of collagen in cartilage of intervertebral disk.

Author

Berthet C, Hulmes DJ, Miller A, and Timmins PA

Subjects

Animals, Glycosaminoglycans, Neutrons, Protein Conformation, Proteoglycans, Scattering, Radiation, Swine, X-Ray Diffraction, Collagen, Intervertebral Disc ultrastructure

Abstract

Small-angle x-ray and neutron diffraction patterns have been obtained from the annulus fibrosus of porcine intervertebral disk. These show that the collagen in this tissue is modified compared with that in tendon.

Published

1978

50. The location of DNA in complexes of recA protein with double-stranded DNA. A neutron scattering study.

Author

DiCapua E, Schnarr M, and Timmins PA

Subjects

Binding Sites, Deuterium, Escherichia coli, Models, Chemical, Molecular Structure, Neutrons, Scattering, Radiation, DNA, Bacterial, Rec A Recombinases

Abstract

Purified recA protein is found as rodlike homopolymers, and it forms filamentous complexes with double-stranded DNA that are stable in the presence of ATP gamma S, a nonhydrolyzable analogue of ATP. The structure of these filaments has been described in some detail by electron microscopy. Here we confirm the mass per length of 6.5 recA/100 A in solution by small-angle neutron scattering and extend the analysis to homopolymers of recA protein, finding a mass per length of about 7 recA/100 A and a radial mass distribution (cross-sectional radius of gyration) significantly different for the two filaments. The models proposed so far for the structure of the complex have placed the DNA in the center of the filament. Here we verify this assumption using small-angle neutron scattering to locate the DNA in the complexes, exploiting the contrast variation method in D2O/H2O mixtures. Model calculations show that the natural contrast difference between DNA and protein is not sufficient to locate the DNA (which accounts for only 4.7% of the mass in the complex). When deuterated DNA is used, the contrast difference is enhanced, and model calculations and experiment then converge, indicating that the DNA is indeed near the axis of the complex.

Published

1989